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US20090181994A1 - Triazole derivatives as inhibitors of 11-beta-hydroxysteroid dehydrogenase-1 - Google Patents

Triazole derivatives as inhibitors of 11-beta-hydroxysteroid dehydrogenase-1 Download PDF

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US20090181994A1
US20090181994A1 US12/364,902 US36490209A US2009181994A1 US 20090181994 A1 US20090181994 A1 US 20090181994A1 US 36490209 A US36490209 A US 36490209A US 2009181994 A1 US2009181994 A1 US 2009181994A1
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alkyl
group
independently selected
unsubstituted
heteroaryl
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US12/364,902
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Sherman T. Waddell
Gina M. Santorelli
Milana M. Maletic
Aaron H. Leeman
Xin Gu
Donald W. Graham
James M. Balkovec
Susan D. Aster
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Merck Sharp and Dohme LLC
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Merck and Co Inc
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Assigned to MERCK SHARP & DOHME CORP. reassignment MERCK SHARP & DOHME CORP. CHANGE OF NAME (SEE DOCUMENT FOR DETAILS). Assignors: MERCK & CO., INC.
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    • C07D249/00Heterocyclic compounds containing five-membered rings having three nitrogen atoms as the only ring hetero atoms
    • C07D249/02Heterocyclic compounds containing five-membered rings having three nitrogen atoms as the only ring hetero atoms not condensed with other rings
    • C07D249/081,2,4-Triazoles; Hydrogenated 1,2,4-triazoles
    • AHUMAN NECESSITIES
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    • A61P3/00Drugs for disorders of the metabolism
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    • AHUMAN NECESSITIES
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    • C07D401/02Heterocyclic compounds containing two or more hetero rings, having nitrogen atoms as the only ring hetero atoms, at least one ring being a six-membered ring with only one nitrogen atom containing two hetero rings
    • C07D401/04Heterocyclic compounds containing two or more hetero rings, having nitrogen atoms as the only ring hetero atoms, at least one ring being a six-membered ring with only one nitrogen atom containing two hetero rings directly linked by a ring-member-to-ring-member bond
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    • C07D417/02Heterocyclic compounds containing two or more hetero rings, at least one ring having nitrogen and sulfur atoms as the only ring hetero atoms, not provided for by group C07D415/00 containing two hetero rings
    • C07D417/08Heterocyclic compounds containing two or more hetero rings, at least one ring having nitrogen and sulfur atoms as the only ring hetero atoms, not provided for by group C07D415/00 containing two hetero rings linked by a carbon chain containing alicyclic rings

Definitions

  • the present invention relates to triazole derivatives as inhibitors of the enzyme 11-beta-hydroxysteroid dehydrogenase Type I (11 ⁇ -HSD-1 or HSD-1) and methods of treatment certain conditions using such compounds.
  • the compounds of the present invention are useful for the treatment of diabetes, such as non-insulin dependent Type 2 diabetes mellitus (NIDDM), insulin resistance, obesity, lipid disorders, hypertension, and other diseases and conditions.
  • NIDDM non-insulin dependent Type 2 diabetes mellitus
  • Type 1 diabetes or insulin-dependent diabetes mellitus (IDDM), in which patients produce little or no insulin, the hormone which regulates glucose utilization
  • IDDM insulin-dependent diabetes mellitus
  • Type 2 diabetes or noninsulin-dependent diabetes mellitus (NIDDM)
  • Type 1 diabetes is typically treated with exogenous insulin administered via injection.
  • Type 2 diabetics often develop “insulin resistance”, such that the effect of insulin in stimulating glucose and lipid metabolism in the main insulin-sensitive tissues, namely, muscle, liver and adipose tissues, is diminished.
  • Patients who are insulin resistant but not diabetic have elevated insulin levels that compensate for their insulin resistance, so that serum glucose levels are not elevated.
  • the plasma insulin levels even when they are elevated, are insufficient to overcome the pronounced insulin resistance, resulting in hyperglycemia.
  • Insulin resistance is primarily due to a receptor binding defect that is not yet completely understood. Resistance to insulin results in insufficient activation of glucose uptake, diminished oxidation of glucose and storage of glycogen in muscle, inadequate insulin repression of lipolysis in adipose tissue and inadequate glucose production and secretion by the liver.
  • Persistent or uncontrolled hyperglycemia that occurs in diabetics is associated with increased morbidity and premature mortality.
  • Abnormal glucose homeostasis is also associated both directly and indirectly with obesity, hypertension and alterations in lipid, lipoprotein and apolipoprotein metabolism.
  • Type 2 diabetics are at increased risk of developing cardiovascular complications, e.g., atherosclerosis, coronary heart disease, stroke, peripheral vascular disease, hypertension, nephropathy, neuropathy and retinopathy. Therefore, therapeutic control of glucose homeostasis, lipid metabolism, obesity and hypertension are critically important in the clinical management and treatment of diabetes mellitus.
  • Syndrome X Syndrome X or Metabolic Syndrome is characterized by insulin resistance, along with abdominal obesity, hyperinsulinemia, high blood pressure, low HDL and high VLDL. These patients, whether or not they develop overt diabetes mellitus, are at increased risk of developing the cardiovascular complications listed above.
  • Treatment of Type 2 diabetes typically includes physical exercise and dieting.
  • Increasing the plasma level of insulin by administration of sulfonylureas (e.g. tolbutamide and glipizide) or meglitinide which stimulate the pancreatic ⁇ -cells to secrete more insulin, and/or by injection of insulin when sulfonylureas or meglitinide become ineffective, can result in insulin concentrations high enough to stimulate insulin-resistant tissues.
  • sulfonylureas e.g. tolbutamide and glipizide
  • meglitinide which stimulate the pancreatic ⁇ -cells to secrete more insulin
  • injection of insulin when sulfonylureas or meglitinide become ineffective
  • Biguanides increase insulin sensitivity, resulting in some correction of hyperglycemia.
  • biguanides e.g., phenformin and metformin, cause lactic acidosis, nausea and diarrhea.
  • the glitazones form a newer class of compounds with the potential for ameliorating hyperglycemia and other symptoms of Type 2 diabetes. These agents substantially increase insulin sensitivity in muscle, liver and adipose tissue, resulting in partial or complete correction of the elevated plasma levels of glucose substantially without causing hypoglycemia.
  • the glitazones that are currently marketed are agonists of the peroxisome proliferator activated receptor (PPAR) gamma subtype.
  • PPAR-gamma agonism is generally believed to be responsible for the improved insulin sensitization that is observed with the glitazones.
  • Newer PPAR agonists that are being developed for treatment of Type 2 diabetes and/or dyslipidemia are agonists of one or more of the PPAR alpha, gamma and delta subtypes.
  • PPAR alpha, gamma and delta subtypes For a review of insulin-sensitizing agents and other mechanisms for the treatment of Type 2 diabetes, see M. Tadayyon and S. A. Smith, “Insulin sensitisation in the treatment of Type 2 diabetes,” Expert Opin. Investig. Drugs, 12: 307-324 (2003).
  • the present invention meets this and other needs.
  • the present invention relates to bicyclo[2.2.2]-oct-1-yl-1,2,4-triazoles of structural formula I
  • bicyclo[2.2.2]-octyltriazole derivatives are effective as inhibitors of 11 ⁇ -hydroxysteroid dehydrogenase type 1 (11 ⁇ -HSD1). They are therefore useful for the treatment, control or prevention of disorders responsive to the inhibition of 11 ⁇ -HSD1, such as Type 2 diabetes, lipid disorders, obesity, atherosclerosis, and Metabolic Syndrome.
  • the present invention also relates to pharmaceutical compositions comprising the compounds of the present invention and a pharmaceutically acceptable carrier.
  • the present invention also relates to methods for the treatment, control, or prevention of disorders, diseases, or conditions responsive to inhibition of 11 ⁇ -HSD1 in a subject in need thereof by administering the compounds and pharmaceutical compositions of the present invention.
  • the present invention also relates to methods for the treatment or control of Type 2 diabetes, obesity, lipid disorders, atherosclerosis, and Metabolic Syndrome by administering the compounds and pharmaceutical compositions of the present invention.
  • the present invention also relates to methods for treating obesity by administering the compounds of the present invention in combination with a therapeutically effective amount of another agent known to be useful to treat the condition.
  • the present invention also relates to methods for treating Type 2 diabetes by administering the compounds of the present invention in combination with a therapeutically effective amount of another agent known to be useful to treat the condition.
  • the present invention also relates to methods for treating atherosclerosis by administering the compounds of the present invention in combination with a therapeutically effective amount of another agent known to be useful to treat the condition.
  • the present invention also relates to methods for treating lipid disorders by administering the compounds of the present invention in combination with a therapeutically effective amount of another agent known to be useful to treat the condition.
  • the present invention also relates to methods for treating Metabolic Syndrome by administering the compounds of the present invention in combination with a therapeutically effective amount of another agent known to be useful to treat the condition.
  • the present invention is also concerned with the use of the compounds of structural formula I for the treatment hyperglycemia, insulin resistance, Type 2 diabetes, lipid disorders, obesity, atherosclerosis, and Metabolic Syndrome.
  • the present invention also provides for the use of the compounds of structural formula I in the manufacture of a medicament for use in the treatment of hyperglycemia, insulin resistance, Type 2 diabetes, lipid disorders, obesity, atherosclerosis, and Metabolic Syndrome.
  • the present invention is concerned with bicyclo[2.2.2]-oct-1-yl-1,2,4-triazole derivatives useful as inhibitors of 11 ⁇ -HSD1.
  • Compounds of the present invention are described by structural formula I:
  • R 1 is selected from the group consisting of
  • R 2 is selected from the group consisting of
  • each R 4 is independently selected from the group consisting of
  • R 3 is selected from the group consisting of
  • R 5 and R 8 are each independently selected from the group consisting of
  • aryl, heteroaryl, cycloalkyl, and heterocyclyl are unsubstituted or substituted with one to three substituents independently selected from halogen, hydroxy, C 1-4 alkyl, trifluoromethyl, trifluoromethoxy, and C 1-4 alkoxy; and wherein any methylene (CH 2 ) carbon atom in R 5 and R 8 is unsubstituted or substituted with one to two groups independently selected from halogen, hydroxy, and C 1-4 alkyl; or two substituents when on the same methylene (CH 2 ) carbon atom are taken together with the carbon atom to which they are attached to form a cyclopropyl group; each R 6 is independently selected from the group consisting of
  • alkyl and cycloalkyl are unsubstituted or substituted with one to five substituents independently selected from halogen, oxo, C 1-4 alkoxy, C 1-4 alkylthio, hydroxy, amino; and aryl and heteroaryl are unsubstituted or substituted with one to three substituents independently selected from cyano, halogen, hydroxy, amino, carboxy, trifluoromethyl, trifluoromethoxy, C 1-4 alkyl, and C 1-4 alkoxy; or two R 6 groups together with the atom to which they are attached form a 5- to 8-membered mono- or bicyclic ring system optionally containing an additional heteroatom selected from O, S, and NC 1-4 alkyl; and each R 7 is hydrogen or R 6 .
  • R 2 is cyclopropyl, C 1-3 alkyl, or C 2-3 alkenyl and R 1 is phenyl or naphthyl in which phenyl and naphthyl are unsubstituted or substituted with one to three substituents independently selected from R 5 .
  • R 5 is selected from the group consisting of halogen, hydroxy, trifluoromethyl, trifluoromethoxy, C 1-3 alkyl, C 1-3 alkoxy, C 1-3 alkylthio, and C 1-3 alkylsulfonyl.
  • R 2 is methyl and R 4 is hydrogen.
  • X is a single bond
  • R 1 is phenyl or naphthyl in which phenyl and naphthyl are unsubstituted or substituted with one to three substituents independently selected from R 5
  • R 2 is cyclopropyl, C 1-3 alkyl, or C 2-3 alkenyl
  • R 3 is C 1-6 alkyl unsubstituted or substituted with one to three substituents independently selected from R 8 and oxo.
  • R 5 is selected from the group consisting of halogen, hydroxy, trifluoromethyl, trifluoromethoxy, C 1-3 alkyl, C 1-3 alkoxy, C 1-3 alkylthio, and C 1-3 alkylsulfonyl.
  • R 2 is methyl and R 4 is hydrogen.
  • R 8 is selected from the group consisting of halogen, hydroxy, oxo, C 1-4 alkoxy, C 1-4 alkylthio, C 1-4 alkylsulfinyl, C 1-4 alkylsulfonyl, and phenyl unsubstituted or substituted with one to three groups independently selected from halogen and trifluoromethyl.
  • R 2 is methyl and R 4 is hydrogen.
  • R 5 is selected from the group consisting of halogen, hydroxy, trifluoromethyl, trifluoromethoxy, C 1-3 alkyl, C 1-3 alkoxy, C 1-3 alkylthio, and C 1-3 alkylsulfonyl; and R 8 is selected from the group consisting of halogen, hydroxy, oxo, C 1-4 alkoxy, C 1-4 alkylthio, C 1-4 alkylsulfonyl, and phenyl unsubstituted or substituted with one to three groups independently selected from halogen and trifluoromethyl.
  • R 2 is methyl and R 4 is hydrogen.
  • X is a single bond
  • R 1 is phenyl or naphthyl in which phenyl and naphthyl are unsubstituted or substituted with one to three substituents independently selected from R 5
  • R 2 is cyclopropyl, C 1-3 alkyl, or C 2-3 alkenyl
  • R 3 is phenyl or heteroaryl wherein phenyl and heteroaryl are unsubstituted or substituted with one with one to three substituents independently selected from R 5 .
  • R 2 is methyl and R 4 is hydrogen.
  • R 3 is phenyl unsubstituted or substituted with one with one to three substituents independently selected from R 5 .
  • R 5 is selected from the group consisting of halogen, hydroxy, trifluoromethyl, trifluoromethoxy, C 1-3 alkyl, C 1-3 alkoxy, C 1-3 alkylthio, and C 1-3 alkylsulfonyl.
  • R 2 is methyl and R 4 is hydrogen.
  • R 3 is oxadiazolyl, unsubstituted or substituted with one with one to two substituents independently selected from R 5 .
  • R 5 is phenyl unsubstituted or substituted with one to three substituents independently selected from halogen, hydroxy, C 1-4 alkyl, trifluoromethyl, trifluoromethoxy, and C 1-4 alkoxy.
  • R 2 is methyl and R 4 is hydrogen.
  • Alkyl as well as other groups having the prefix “alk”, such as alkoxy and alkanoyl, means carbon chains which may be linear or branched, and combinations thereof, unless the carbon chain is defined otherwise.
  • alkyl groups include methyl, ethyl, propyl, isopropyl, butyl, sec- and tert-butyl, pentyl, hexyl, heptyl, octyl, nonyl, and the like.
  • the term alkyl also includes cycloalkyl groups, and combinations of linear or branched alkyl chains combined with cycloalkyl structures. When no number of carbon atoms is specified, C 1-6 is intended.
  • alkenyl means carbon chains which contain at least one carbon-carbon double bond, and which may be linear or branched or combinations thereof, unless the carbon chain is defined otherwise.
  • alkenyl include vinyl, allyl, isopropenyl, pentenyl, hexenyl, heptenyl, 1-propenyl, 2-butenyl, 2-methyl-2-butenyl, and the like.
  • the specified number of carbon atoms permits, e.g., from C 5-10
  • the term alkenyl also includes cycloalkenyl groups, and combinations of linear, branched and cyclic structures. When no number of carbon atoms is specified, C 2-6 is intended.
  • Alkynyl means carbon chains which contain at least one carbon-carbon triple bond, and which may be linear or branched or combinations thereof. Examples of alkynyl include ethynyl, propargyl, 3-methyl-1-pentynyl, 2-heptynyl, and the like.
  • Cycloalkyl is a subset of alkyl and means a saturated carbocyclic ring having a specified number of carbon atoms. Examples of cycloalkyl include cyclopropyl, cyclobutyl, cyclopentyl, cyclohexyl, cycloheptyl, cyclooctyl, and the like. A cycloalkyl group generally is monocyclic unless stated otherwise. Cycloalkyl groups are saturated unless otherwise defined.
  • alkoxy refers to straight or branched chain alkoxides of the number of carbon atoms specified (e.g., C 1-6 alkoxy), or any number within this range [i.e., methoxy (MeO—), ethoxy, isopropoxy, etc.].
  • alkylthio refers to straight or branched chain alkylsulfides of the number of carbon atoms specified (e.g., C 1-6 alkylthio), or any number within this range [i.e., methylthio (MeS—), ethylthio, isopropylthio, etc.].
  • alkylamino refers to straight or branched alkylamines of the number of carbon atoms specified (e.g., C 1-6 alkylamino), or any number within this range [i.e., methylamino, ethylamino, isopropylamino, t-butylamino, etc.].
  • alkylsulfonyl refers to straight or branched chain alkylsulfones of the number of carbon atoms specified (e.g., C 1-6 alkylsulfonyl), or any number within this range [i.e., methylsulfonyl (MeSO 2 —), ethylsulfonyl, isopropylsulfonyl, etc.].
  • alkylsulfinyl refers to straight or branched chain alkylsulfoxides of the number of carbon atoms specified (e.g., C 1-6 alkylsulfinyl), or any number within this range [i.e., methylsulfinyl (MeSO—), ethylsulfinyl, isopropylsulfinyl, etc.].
  • alkyloxycarbonyl refers to straight or branched chain esters of a carboxylic acid derivative of the present invention of the number of carbon atoms specified (e.g., C 1-6 alkyloxycarbonyl), or any number within this range [i.e., methyloxycarbonyl (MeOCO—), ethyloxycarbonyl, or butyloxycarbonyl].
  • Aryl means a mono- or polycyclic aromatic ring system containing carbon ring atoms.
  • the preferred aryls are monocyclic or bicyclic 6-10 membered aromatic ring systems. Phenyl and naphthyl are preferred aryls. The most preferred aryl is phenyl.
  • Heterocycle and “heterocyclyl” refer to saturated or unsaturated non-aromatic rings or ring systems containing at least one heteroatom selected from O, S and N, further including the oxidized forms of sulfur, namely SO and SO 2 .
  • heterocycles include tetrahydrofuran (THF), dihydrofuran, 1,4-dioxane, morpholine, 1,4-dithiane, piperazine, piperidine, 1,3-dioxolane, imidazolidine, imidazoline, pyrroline, pyrrolidine, tetrahydropyran, dihydropyran, oxathiolane, dithiolane, 1,3-dioxane, 1,3-dithiane, oxathiane, thiomorpholine, and the like.
  • THF tetrahydrofuran
  • dihydrofuran 1,4-dioxane
  • morpholine 1,4-dithiane
  • 1,4-dithiane piperazine
  • piperidine 1,3-dioxolane
  • imidazolidine imidazoline
  • pyrroline pyrrolidine
  • tetrahydropyran dihydropyran
  • Heteroaryl means an aromatic or partially aromatic heterocycle that contains at least one ring heteroatom selected from O, S and N. Heteroaryls thus includes heteroaryls fused to other kinds of rings, such as aryls, cycloalkyls and heterocycles that are not aromatic.
  • heteroaryl groups include: pyrrolyl, isoxazolyl, isothiazolyl, pyrazolyl, pyridyl, oxazolyl, oxadiazolyl, thiadiazolyl, thiazolyl, imidazolyl, triazolyl, tetrazolyl, furyl, triazinyl, thienyl, pyrimidyl, benzisoxazolyl, benzoxazolyl, benzothiazolyl, benzothiadiazolyl, dihydrobenzofuranyl, indolinyl, pyridazinyl, indazolyl, isoindolyl, dihydrobenzothienyl, indolizinyl, cinnolinyl, phthalazinyl, quinazolinyl, naphthyridinyl, carbazolyl, benzodioxolyl, quinoxalinyl, purinyl,
  • Halogen refers to fluorine, chlorine, bromine and iodine. Chlorine and fluorine are generally preferred. Fluorine is most preferred when the halogens are substituted on an alkyl or alkoxy group (e.g. CF 3 O and CF 3 CH 2 O).
  • composition as in pharmaceutical composition, is intended to encompass a product comprising the active ingredient(s), and the inert ingredient(s) that make up the carrier, as well as any product which results, directly or indirectly, from combination, complexation or aggregation of any two or more of the ingredients, or from dissociation of one or more of the ingredients, or from other types of reactions or interactions of one or more of the ingredients.
  • pharmaceutical compositions of the present invention encompass any composition made by admixing a compound of the present invention and a pharmaceutically acceptable carrier.
  • administering should be understood to mean providing a compound of the invention or a prodrug of a compound of the invention to the individual in need.
  • Compounds of structural formula I may contain one or more asymmetric centers and can thus occur as racemates and racemic mixtures, single enantiomers, diastereomeric mixtures and individual diastereomers. The present invention is meant to comprehend all such isomeric forms of the compounds of structural formula I.
  • Some of the compounds described herein may exist as tautomers such as keto-enol tautomers.
  • the individual tautomers, as well as mixtures thereof, are encompassed within the compounds of structural formula I.
  • Compounds of structural formula I may be separated into their individual diastereoisomers by, for example, fractional crystallization from a suitable solvent, for example methanol or ethyl acetate or a mixture thereof, or via chiral chromatography using an optically active stationary phase.
  • Absolute stereochemistry may be determined by X-ray crystallography of crystalline products or crystalline intermediates which are derivatized, if necessary, with a reagent containing an asymmetric center of known absolute configuration.
  • any stereoisomer of a compound of the general structural formula I may be obtained by stereospecific synthesis using optically pure starting materials or reagents of known absolute configuration.
  • a pharmaceutical composition comprising a compound in accordance with structural formula I, or a pharmaceutically acceptable salt or solvate thereof, in combination with a pharmaceutically acceptable carrier.
  • solvate is meant a hydrate, an alcoholate, or other solvate of crystallization.
  • a method of treating hyperglycemia, diabetes or insulin resistance in a mammalian patient in need of such treatment comprises administering to said patient an effective amount of a compound in accordance with structural formula I or a pharmaceutically salt or solvate thereof.
  • a method of treating non-insulin dependent (Type 2) diabetes mellitus in a mammalian patient in need of such treatment comprising administering to the patient an anti-diabetic effective amount of a compound in accordance with structural formula I.
  • a method of treating obesity in a mammalian patient in need of such treatment comprising administering to said patient a compound in accordance with structural formula I in an amount that is effective to treat obesity.
  • a method of treating Metabolic Syndrome in a mammalian patient in need of such treatment comprising administering to said patient a compound in accordance with structural formula I in an amount that is effective to treat Metabolic Syndrome.
  • a method of treating a lipid disorder selected from the group consisting of dyslipidemia, hyperlipidemia, hypertriglyceridemia, hypercholesterolemia, low HDL, and high LDL in a mammalian patient in need of such treatment comprising administering to said patient a compound in accordance with structural formula I in an amount that is effective to treat said lipid disorder.
  • a method of treating atherosclerosis in a mammalian patient in need of such treatment comprising administering to said patient a compound in accordance with structural formula I in an amount effective to treat atherosclerosis.
  • insulin sensitizing agents selected from the group consisting of (i) PPAR ⁇ agonists, (ii) PPAR ⁇ agonists, (iii) PPAR ⁇ / ⁇ dual agonists, and (iv) biguanides;
  • PACAP PACAP, PACAP mimetics, and PACAP receptor 3 agonists
  • antihypertensives including those acting on the angiotensin or renin systems, such as angiotensin converting enzyme inhibitors, angiotensin II receptor antagonists or renin inhibitors, such as captopril, cilazapril, enalapril, fosinopril, lisinopril, quinapril, ramapril, zofenopril, candesartan, cilexetil, eprosartan, irbesartan, losartan, tasosartan, telmisartan, and valsartan;
  • said compounds being administered to the patient in an amount that is effective to treat said condition.
  • Dipeptidyl peptidase-IV inhibitors that can be combined with compounds of structural formula I include those disclosed in WO 03/004498 (16 Jan. 2003); WO 03/004496 (16 Jan. 2003); EP 1 258 476 (20 Nov. 2002); WO 02/083128 (24 Oct. 2002); WO 02/062764 (15 Aug. 2002); WO 03/000250 (3 Jan. 2003); WO 03/002530 (9 Jan. 2003); WO 03/002531 (9
  • Specific DP-IV inhibitor compounds include isoleucine thiazolidide; NVP-DPP728; P32/98; and LAF 237.
  • Antiobesity compounds that can be combined with compounds of structural formula I include fenfluramine, dexfenfluramine, phentermine, sibutramine, orlistat, neuropeptide Y 1 or Y 5 antagonists, cannabinoid CB1 receptor antagonists or inverse agonists, melanocortin receptor agonists, in particular, melanocortin-4 receptor agonists, ghrelin antagonists, and melanin-concentrating hormone (MCH) receptor antagonists.
  • MCH melanin-concentrating hormone
  • Neuropeptide Y5 antagonists that can be combined with compounds of structural formula I include those disclosed in U.S. Pat. No. 6,335,345 (1 Jan. 2002) and WO 01/14376 (1 Mar. 2001); and specific compounds identified as GW 59884A; GW 569180A; LY366377; and CGP-71683A.
  • Cannabinoid CB1 receptor antagonists that can be combined with compounds of formula I include those disclosed in PCT Publication WO 03/007887; U.S. Pat. No. 5,624,941, such as rimonabant; PCT Publication WO 02/076949, such as SLV-319; U.S. Pat. No. 6,028,084; PCT Publication WO 98/41519; PCT Publication WO 00/10968; PCT Publication WO 99/02499; U.S. Pat. No. 5,532,237; and U.S. Pat. No. 5,292,736.
  • Melanocortin receptor agonists that can be combined with compounds of structural formula I include those disclosed in WO 03/009847 (6 Feb. 2003); WO 02/068388 (6 Sep. 2002); WO 99/64002 (16 Dec. 1999); WO 00/74679 (14 Dec. 2000); WO 01/70708 (27 Sep. 2001); and WO 01/70337 (27 Sep. 2001) as well as those disclosed in J. D. Speake et al., “Recent advances in the development of melanocortin-4 receptor agonists, Expert Opin. Ther. Patents, 12: 1631-1638 (2002).
  • a method of treating a condition selected from the group consisting of hypercholesterolemia, atherosclerosis, low HDL levels, high LDL levels, hyperlipidemia, hypertriglyceridemia, and dyslipidemia, in a mammalian patient in need of such treatment comprising administering to the patient a therapeutically effective amount of a compound as defined in structural formula I and an HMG-CoA reductase inhibitor.
  • a method of treating a condition selected from the group consisting of hypercholesterolemia, atherosclerosis, low HDL levels, high LDL levels, hyperlipidemia, hypertriglyceridemia and dyslipidemia, in a mammalian patient in need of such treatment is disclosed, wherein the HMG-CoA reductase inhibitor is a statin.
  • a method of treating a condition selected from the group consisting of hypercholesterolemia, atherosclerosis, low HDL levels, high LDL levels, hyperlipidemia, hypertriglyceridemia and dyslipidemia, in a mammalian patient in need of such treatment is disclosed, wherein the HMG-CoA reductase inhibitor is a statin selected from the group consisting of lovastatin, simvastatin, pravastatin, cerivastatin, fluvastatin, atorvastatin, itavastatin, and rosuvastatin.
  • a method of reducing the risk of developing a condition selected from the group consisting of hypercholesterolemia, atherosclerosis, low HDL levels, high LDL levels, hyperlipidemia, hypertriglyceridemia and dyslipidemia, and the sequelae of such conditions comprising administering to a mammalian patient in need of such treatment a therapeutically effective amount of a compound as defined in structural formula I and an HMG-CoA reductase inhibitor.
  • a method for delaying the onset or reducing the risk of developing atherosclerosis in a human patient in need of such treatment comprising administering to said patient an effective amount of a compound as defined in structural formula I and an HMG-CoA reductase inhibitor.
  • HMG-CoA reductase inhibitor is a statin.
  • the HMG-Co A reductase inhibitor is a statin selected from the group consisting of: lovastatin, simvastatin, pravastatin, cerivastatin, fluvastatin, atorvastatin, itavastatin, and rosuvastatin.
  • statin is simvastatin.
  • a method for delaying the onset or reducing the risk of developing atherosclerosis in a human patient in need of such treatment is disclosed, wherein the HMG-CoA reductase inhibitor is a statin and further comprising administering a cholesterol absorption inhibitor.
  • a method for delaying the onset or reducing the risk of developing atherosclerosis in a human patient in need of such treatment is disclosed, wherein the HMG-Co A reductase inhibitor is a statin and the cholesterol absorption inhibitor is ezetimibe.
  • composition which comprises
  • insulin sensitizing agents selected from the group consisting of (i) PPAR ⁇ agonists; (ii) PPAR ⁇ agonists, (iii) PPAR ⁇ / ⁇ dual agonists, and (iv) biguanides;
  • PACAP PACAP, PACAP mimetics, and PACAP receptor 3 agonists
  • k) cholesterol lowering agents selected from the group consisting of (i) HMG-CoA reductase inhibitors, (ii) sequestrants, (iii) nicotinyl alcohol, nicotinic acid or a salt thereof, (iv) inhibitors of cholesterol absorption, (v) acyl CoA:cholesterol acyltransferase inhibitors, and (vi) anti-oxidants;
  • antihypertensives including those acting on the angiotensin or renin systems, such as angiotensin converting enzyme inhibitors, angiotensin II receptor antagonists or renin inhibitors, such as captopril, cilazapril, enalapril, fosinopril, lisinopril, quinapril, ramapril, zofenopril, candesartan, cilexetil, eprosartan, irbesartan, losartan, tasosartan, telmisartan, and valsartan; and
  • the compounds of the present invention may be administered in the form of a pharmaceutically acceptable salt.
  • pharmaceutically acceptable salt refers to salts prepared from pharmaceutically acceptable non-toxic bases or acids including inorganic or organic bases and inorganic or organic acids. Salts of basic compounds encompassed within the term “pharmaceutically acceptable salt” refer to non-toxic salts of the compounds of this invention which are generally prepared by reacting the free base with a suitable organic or inorganic acid.
  • Representative salts of basic compounds of the present invention include, but are not limited to, the following: acetate, benzenesulfonate, benzoate, bicarbonate, bisulfate, bitartrate, borate, bromide, camsylate, carbonate, chloride, clavulanate, citrate, dihydrochloride, edetate, edisylate, estolate, esylate, fumarate, gluceptate, gluconate, glutamate, glycollylarsanilate, hexylresorcinate, hydrabamine, hydrobromide, hydrochloride, hydroxynaphthoate, iodide, isothionate, lactate, lactobionate, laurate, malate, maleate, mandelate, mesylate, methylbromide, methylnitrate, methylsulfate, mucate, napsylate, nitrate, N-methylglucamine ammonium salt,
  • suitable pharmaceutically acceptable salts thereof include, but are not limited to, salts derived from inorganic bases including aluminum, ammonium, calcium, copper, ferric, ferrous, lithium, magnesium, manganic, mangamous, potassium, sodium, zinc, and the like. Particularly preferred are the ammonium, calcium, magnesium, potassium, and sodium salts.
  • Salts derived from pharmaceutically acceptable organic non-toxic bases include salts of primary, secondary, and tertiary amines, cyclic amines, and basic ion-exchange resins, such as arginine, betaine, caffeine, choline, N,N-dibenzylethylenediamine, diethylamine, 2-diethylaminoethanol, 2-dimethylaminoethanol, ethanolamine, ethylenediamine, N-ethylmorpholine, N-ethylpiperidine, glucamine, glucosamine, histidine, hydrabamine, isopropylamine, lysine, methylglucamine, morpholine, piperazine, piperidine, polyamine resins, procaine, purines, theobromine, triethylamine, trimethylamine, tripropylamine, tromethamine, and the like.
  • basic ion-exchange resins such as arginine, betaine, caffeine, cho
  • esters of carboxylic acid derivatives such as methyl, ethyl, or pivaloyloxymethyl, or acyl derivatives of alcohols, such as acetate or maleate, can be employed. Included are those esters and acyl groups known in the art for modifying the solubility or hydrolysis characteristics for use as sustained-release or prodrug formulations.
  • references to the compounds of structural formula I are meant to also include the pharmaceutically acceptable salts, and also salts that are not pharmaceutically acceptable when they are used as precursors to the free compounds or their pharmaceutically acceptable salts or in other synthetic manipulations.
  • the compounds described herein are selective inhibitors of the 11 ⁇ -HSD1 enzyme.
  • the present invention relates to the use of the 11 ⁇ -HSD1 inhibitors for inhibiting the reductase activity of 11 ⁇ -hydroxysteroid dehydrogenase, which is responsible for the conversion of cortisone to cortisol.
  • Excess cortisol is associated with numerous disorders, including NIDDM, obesity, dyslipidemia, insulin resistance and hypertension.
  • Administration of the compounds of the present invention decreases the level of cortisol and other 11 ⁇ -hydroxysteroids in target tissues, thereby reducing the effects of excessive amounts of cortisol and other 11 ⁇ -hydroxysteroids.
  • Inhibition of 11 ⁇ -HSD1 can be used to treat and control diseases mediated by abnormally high levels of cortisol and other 11 ⁇ -hydroxysteroids, such as NIDDM, obesity, hypertension and dyslipidemia. Inhibition of 11 ⁇ -HSD1 activity in the brain such as to lower cortisol levels may also be useful to treat or reduce anxiety, depression, and cognitive impairment.
  • the present invention includes the use of an 11 ⁇ -HSD1 inhibitor for the treatment, control, amelioration, prevention, delaying the onset of or reducing the risk of developing the diseases and conditions that are described herein, as mediated by excess or uncontrolled amounts of cortisol and/or other corticosteroids in a mammalian patient, particularly a human, by the administration of an effective amount of a compound of structural formula I or a pharmaceutically acceptable salt or solvate thereof.
  • Inhibition of the 11 ⁇ -HSD1 enzyme limits the conversion of cortisone, which is normally inert, to cortisol, which can cause or contribute to the symptoms of these diseases and conditions if present in excessive amounts.
  • the compounds of this invention are selective inhibitors of 11 ⁇ -HSD1 over 11 ⁇ -HSD2. While the inhibition of 11 ⁇ -HSD1 is useful for reducing cortisol levels and treating conditions related thereto, inhibition of 11 ⁇ -HSD2 is associated with serious side effects, such as hypertension.
  • Cortisol is an important and well recognized anti-inflammatory hormone, which also acts as an antagonist to the action of insulin in the liver, such that insulin sensitivity is reduced, resulting in increased gluconeogenesis and elevated levels of glucose in the liver.
  • Patients who already have impaired glucose tolerance have a greater probability of developing Type 2 diabetes in the presence of abnormally high levels of cortisol.
  • Administration of a therapeutically effective amount of an 11 ⁇ -HSD1 inhibitor is effective in treating, controlling and ameliorating the symptoms of NIDDM, and administration of a therapeutically effective amount of an 11 ⁇ -HSD1 inhibitor on a regular basis delays or prevents the onset of NIDDM, particularly in humans.
  • compounds of the present invention By reducing insulin resistance and maintaining serum glucose at normal concentrations, compounds of the present invention also have utility in the treatment and prevention of conditions that accompany Type II diabetes and insulin resistance, including the Metabolic Syndrome or Syndrome X, obesity, reactive hypoglycemia and diabetic dyslipidemia.
  • Excessive levels of cortisol in the brain may also result in neuronal loss or dysfunction through the potentiation of neurotoxins.
  • Cognitive impairment has been associated with aging, and excess levels of cortisol in the brain. See J. R. Seckl and B. R. Walker, Endocrinology, 2001, 142: 1371-1376, and references cited therein.
  • Administration of an effective amount of an 11 ⁇ -HSD1 inhibitor results in the reduction, amelioration, control or prevention of cognitive impairment associated with aging and of neuronal dysfunction.
  • Inhibitors of 11 ⁇ -HSD1 may also be useful to treat anxiety and depression.
  • inhibition of 113-HSD1 activity and a reduction in the amount of cortisol are beneficial in treating or controlling hypertension. Since hypertension and dyslipidemia contribute to the development of atherosclerosis, administration of a therapeutically effective amount of an 11 ⁇ -HSD1 inhibitor of the present invention may be especially beneficial in treating, controlling, delaying the onset of or preventing atherosclerosis.
  • Glucocorticoids can inhibit bone formation, which can result in a net bone loss.
  • 11 ⁇ -HSD1 has a role in bone resorption. Inhibition of 11 ⁇ -HSD1 is beneficial in preventing bone loss due to osteoporosis. See C. H. Kim et al., J. Endocrinol., 1999, 162: 371-379; C. G. Bellows et al., Bone, 1998, 23: 119-125; and M. S. Cooper et al., Bone, 2000, 27: 375-381.
  • the following diseases, disorders and conditions can be treated, controlled, prevented or delayed, by treatment with the compounds of this invention: (1) hyperglycemia, (2) low glucose tolerance, (3) insulin resistance, (4) obesity, (5) lipid disorders, (6) dyslipidemia, (7) hyperlipidemia, (8) hypertriglyceridemia, (9) hypercholesterolemia, (10) low HDL levels, (11) high LDL levels, (12) atherosclerosis and its sequelae, (13) vascular restenosis, (14) pancreatitis, (15) abdominal obesity, (16) neurodegenerative disease, (17) retinopathy, (18) nephropathy, (19) neuropathy, (20) Metabolic Syndrome, (21) hypertension and other disorders where insulin resistance is a component.
  • the above diseases and conditions can be treated using the compounds of structural formula I, or the compound can be administered to prevent or reduce the risk of developing the diseases and conditions described herein. Since concurrent inhibition of 11 ⁇ -HSD2 may have deleterious side effects or may actually increase the amount of cortisol in the target tissue where reduction of cortisol is desired, selective inhibitors of 11 ⁇ -HSD1 with little or no inhibition of 11 ⁇ -HSD2 are desirable.
  • the 11 ⁇ -HSD1 inhibitors of structural formula I generally have an inhibition constant IC 50 of less than about 500 nM, and preferably less than about 100 nM.
  • the IC 50 ratio for 11 ⁇ -HSD2 to 11 ⁇ -HSD1 of a compound is at least about two or more, and preferably about ten or greater. Even more preferred are compounds with an IC 50 ratio for 11 ⁇ -HSD2 to 11 ⁇ -HSD1 of about 100 or greater.
  • compounds of the present invention ideally demonstrate an inhibition constant IC 50 against 11 ⁇ -HSD2 greater than about 1000 nM, and preferably greater than 5000 nM.
  • Compounds of structural formula I may be used in combination with one or more other drugs in the treatment, prevention, suppression or amelioration of diseases or conditions for which compounds of structural formula I or the other drugs have utility.
  • the combination of the drugs is safer or more effective than either drug alone, or the combination is safer or more effective than would be expected based on the additive properties of the individual drugs.
  • Such other drug(s) may be administered, by a route and in an amount commonly used contemporaneously or sequentially with a compound of structural formula I.
  • a combination product containing such other drug(s) and the compound of structural formula I is preferred.
  • combination therapy also includes therapies in which the compound of structural formula I and one or more other drugs are administered on different overlapping schedules. It is contemplated that when used in combination with other active ingredients, the compound of the present invention or the other active ingredient or both may be used effectively in lower doses than when each is used alone. Accordingly, the pharmaceutical compositions of the present invention include those that contain one or more other active ingredients, in addition to a compound of structural formula I.
  • Examples of other active ingredients that may be administered in combination with a compound of structural formula I, and either administered separately or in the same pharmaceutical composition include, but are not limited to:
  • insulin sensitizing agents including (i) PPAR ⁇ agonists such as the glitazones (e.g. troglitazone, pioglitazone, englitazone, MCC-555, rosiglitazone, and the like) and other PPAR ligands, including PPAR ⁇ / ⁇ dual agonists, such as KRP-297, and PPAR ⁇ agonists such as gemfibrozil, clofibrate, fenofibrate and bezafibrate, and (ii) biguanides, such as metformin and phenformin;
  • PPAR ⁇ agonists such as the glitazones (e.g. troglitazone, pioglitazone, englitazone, MCC-555, rosiglitazone, and the like) and other PPAR ligands, including PPAR ⁇ / ⁇ dual agonists, such as KRP-297, and PPAR ⁇ agonists such as gemfibrozi
  • ⁇ -glucosidase inhibitors such as acarbose
  • glucagon receptor antagonists such as those disclosed in WO 98/04528, WO 99/01423, WO 00/39088 and WO 00/69810;
  • GLP-1 GLP-1, GLP-1 analogs, and GLP-1 receptor agonists such as those disclosed in WO00/42026 and WO00/59887;
  • GIP GIP, GIP mimetics such as those disclosed in WO00/58360, and GIP receptor agonists;
  • PACAP PACAP, PACAP mimetics, and PACAP receptor 3 agonists such as those disclosed in WO 01/23420;
  • k) cholesterol lowering agents such as (i) HMG-CoA reductase inhibitors (lovastatin, simvastatin, pravastatin, cerivastatin, fluvastatin, atorvastatin, itavastatin, rosuvastatin, and other statins), (ii) bile-acid sequestrants (cholestyramine, colestipol, and dialkylaminoalkyl derivatives of a cross-linked dextran), (iii) nicotinyl alcohol, nicotinic acid or a salt thereof, (iv) inhibitors of cholesterol absorption, such as ezetimibe and beta-sitosterol, (v) acyl CoA:cholesterol acyltransferase inhibitors, such as, for example, avasimibe, and (vi) anti-oxidants, such as probucol;
  • HMG-CoA reductase inhibitors lovastatin, simvastatin,
  • (l) antiobesity compounds such as fenfluramine, dexfenfluramine, phentermine, sibutramine, orlistat, neuropeptide Y 1 or Y 5 antagonists, CB1 receptor inverse agonists and antagonists, ⁇ 3 adrenergic receptor agonists, melanocortin-receptor agonists, in particular melanocortin-4 receptor agonists, ghrelin antagonists, and melanin-concentrating hormone (MCH) receptor antagonists;
  • MCH melanin-concentrating hormone
  • agents intended for use in inflammatory conditions other than glucocorticoids such as aspirin, non-steroidal anti-inflammatory drugs, azulfidine, and selective cyclooxygenase-2 inhibitors;
  • antihypertensives including those acting on the angiotensin or renin systems, such as angiotensin converting enzyme inhibitors, angiotensin II receptor antagonists or renin inhibitors, such as captopril, cilazapril, enalapril, fosinopril, lisinopril, quinapril, ramapril, zofenopril, candesartan, cilexetil, eprosartan, irbesartan, losartan, tasosartan, telmisartan, and valsartan.
  • angiotensin converting enzyme inhibitors such as captopril, cilazapril, enalapril, fosinopril, lisinopril, quinapril, ramapril, zofenopril
  • candesartan cilexetil
  • eprosartan irbesartan
  • the above combinations include a compound of structural formula I, or a pharmaceutically acceptable salt or solvate thereof, with one or more other active compounds.
  • Non-limiting examples include combinations of compounds of structural formula I with two or more active compounds selected from biguanides, sulfonylureas, HMG-CoA reductase inhibitors, PPAR agonists, PTP-1B inhibitors, DP-IV inhibitors, and anti-obesity compounds.
  • Any suitable route of administration may be employed for providing a mammal, especially a human, with an effective dose of a compound of the present invention.
  • oral, rectal, topical, parenteral, ocular, pulmonary, nasal and the like may be employed.
  • Dosage forms include tablets, troches, dispersions, suspensions, solutions, capsules, creams, ointments, aerosols and the like.
  • the compound of structural formula I is administered orally.
  • the effective dosage of the active ingredient varies depending on the particular compound employed, the mode of administration, the condition being treated and the severity of the condition. Such dosages may be ascertained readily by a person skilled in the art.
  • the compounds of the invention are administered at a daily dosage of from about 0.1 to about 100 milligram per kilogram (mpk) of body weight, preferably given as a single daily dose or in divided doses about two to six times a day.
  • the total daily dosage thus ranges from about 0.1 mg to about 1000 mg, preferably from about 1 mg to about 50 mg. In the case of a typical 70 kg adult human, the total daily dose will range from about 7 mg to about 350 mg. This dosage may be adjusted to provide the optimal therapeutic response.
  • Another aspect of the present invention relates to a pharmaceutical composition which comprises a compound of structural formula I, or a pharmaceutically acceptable salt or solvate thereof, in combination with a pharmaceutically acceptable carrier.
  • the compound of structural formula I can be combined with the pharmaceutical carrier according to conventional pharmaceutical compounding techniques.
  • Carriers take a wide variety of forms.
  • carriers for oral liquid compositions include, e.g., water, glycols, oils, alcohols, flavoring agents, preservatives, coloring agents and other components used in the manufacture of oral liquid suspensions, elixirs and solutions.
  • Carriers such as starches, sugars and microcrystalline cellulose, diluents, granulating agents, lubricants, binders, disintegrating agents and the like are used to prepare oral solid dosage forms, e.g., powders, hard and soft capsules and tablets. Solid oral preparations are preferred over oral liquids.
  • the oral solid dosage forms may also contain a binder such as gum tragacanth, acacia, corn starch or gelatin; excipients such as dicalcium phosphate; a disintegrating agent such as corn starch, potato starch, alginic acid; a lubricant such as magnesium stearate; and a sweetening agent such as sucrose, lactose or saccharin.
  • a binder such as gum tragacanth, acacia, corn starch or gelatin
  • excipients such as dicalcium phosphate
  • a disintegrating agent such as corn starch, potato starch, alginic acid
  • a lubricant such as magnesium stearate
  • a sweetening agent such as sucrose, lactose or saccharin.
  • Capsules may also contain a liquid carrier such as a fatty oil.
  • tablets may be coated with shellac, sugar or both.
  • Tablets may be coated by standard aqueous or nonaqueous techniques.
  • the typical percentage of active compound in these compositions may, of course, be varied from about 2 percent to about 60 percent on a w/w basis.
  • tablets contain a compound of structural formula I or a salt or hydrate thereof in an amount ranging from as low as about 0.1 mg to as high as about 1.5 g, preferably from as low as about 1.0 mg to as high as about 500 mg, and more preferably from as low as about 10 mg to as high as about 100 mg.
  • Oral liquids such as syrups or elixirs may contain, in addition to the active ingredient, sucrose as a sweetening agent, methyl and propylparabens as preservatives, a dye and a flavoring such as cherry or orange flavor.
  • Parenterals are typically in the form of a solution or suspension, typically prepared with water, and optionally including a surfactant such as hydroxypropylcellulose.
  • Dispersions can be prepared in glycerol, liquid polyethylene glycols and mixtures thereof in oils. Typically preparations that are in diluted form also contain a preservative.
  • the pharmaceutical injectable dosage forms including aqueous solutions and dispersions and powders for the extemporaneous preparation of injectable solutions or dispersions, are also sterile and must be fluid to the extent that easy syringability exists; they must be stable under the conditions of manufacture and storage and are usually preserved.
  • the carrier thus includes the solvent or dispersion medium containing, for example, water, ethanol, polyol (e.g. glycerol, propylene glycol and liquid polyethylene glycol), suitable mixtures thereof, and vegetable oils.
  • SPA Scintillation Proximity Assay
  • Percent inhibition was calculated relative to a non-inhibited control well and IC 50 curves were generated. This assay was similarly applied to 11 ⁇ -HSD2, whereby tritiated cortisol and NAD were used as the substrate and cofactor, respectively.
  • substrate 25 nM 3 H-Cortisone+1.25 mM NADPH in 50 mM HEPES Buffer, pH 7.4
  • the compound was dissolved in DMSO at 10 mM followed by a subsequent 50 fold dilution in DMSO. The diluted material was then titrated 4 fold, seven times. 1 ⁇ L of each titrated compound was then added in duplicate to the substrate.
  • test compound was dosed orally to a mammal and a prescribed time interval was allowed to elapse, usually between 1 and 24 h.
  • Tritiated cortisone was injected intravenously, followed several min later by blood collection.
  • Steroids were extracted from the separated serum and analyzed by HPLC.
  • the relative levels of 3 H-cortisone and its reduction product, 3 H-cortisol were determined for the compound and vehicle-dosed control groups. The absolute conversion, as well as the percentage of inhibition, was calculated from these values.
  • compounds were prepared for oral dosing by dissolving them in vehicle (5% hydroxypropyl-beta-cyclodextrin v/v H 2 O, or equivalent) at the desired concentration to allow dosing at typically 10 mg per kg. Following an overnight fasting, the solutions were dosed to ICR mice (obtained from Charles River) by oral gavage, 0.5 mL per dose per animal, with three animals per test group.
  • vehicle 5% hydroxypropyl-beta-cyclodextrin v/v H 2 O, or equivalent
  • 0.2 mL of 3 ⁇ M 3 H-cortisone in dPBS was injected by tail vein.
  • the animal was caged for two min followed by euthanasia in a CO 2 chamber.
  • the mouse was removed and blood was collected by cardiac puncture.
  • the blood was set aside in a serum separation tube for no less than 30 min at room temperature to allow for adequate coagulation.
  • blood was separated into serum by centrifugation at 3000 ⁇ g, 4° C., for 10 min.
  • the compounds of structural formula I of the present invention can be prepared according to the procedures of the following Schemes and Examples, using appropriate materials and are further exemplified by the following specific examples.
  • the compounds illustrated in the examples are not, however, to be construed as forming the only genus that is considered as the invention.
  • the Examples further illustrate details for the preparation of the compounds of the present invention. Those skilled in the art will readily understand that known variations of the conditions and processes of the following preparative procedures can be used to prepare these compounds.
  • the instant compounds are generally isolated in the their neutral form, but the triazole moeity can be further converted into a pharmaceutically acceptable salt by dissolution in an organic solvent followed by addition of the appropriate acid and subsequent evaporation, precipitation, or crystallization. All temperatures are degrees Celsius unless otherwise noted.
  • Mass spectra (MS) were measured by electrospray ion-mass spectroscopy (ESMS).
  • standard peptide coupling reaction conditions means coupling a carboxylic acid with an amine using an acid activating agent such as EDC, DCC, and BOP in an inert solvent such as dichloromethane in the presence of a catalyst such as HOBT.
  • an acid activating agent such as EDC, DCC, and BOP
  • an inert solvent such as dichloromethane
  • HOBT a catalyst
  • protecting groups for the amine and carboxylic acid functionalities to facilitate the desired reaction and minimize undesired reactions is well documented. Conditions required to remove protecting groups are found in standard textbooks such as Greene, T, and Wuts, P. G. M., Protective Groups in Organic Synthesis , John Wiley & Sons, Inc., New York, N.Y., 1991. Cbz and BOC are commonly used protecting groups in organic synthesis, and their removal conditions are known to those skilled in the art.
  • Reaction Schemes 1-5 illustrate the methods employed in the synthesis of the compounds of the present invention of structural formula I. All substituents are as defined above unless indicated otherwise.
  • Reaction Scheme 1 illustrates a key step in the synthesis of the novel compounds of structural formula I of the present invention.
  • a secondary amide (1-1) (N-Me or N-Et preferred) can be methylated by heating with neat methyl triflate in order to provide an iminoether (1-2).
  • other methylating reagents such as methyl iodide or methyl sulfate may be used neat or in a non-nucleophilic organic solvent.
  • a bicyclo[2.2.2]octane-1-carboxylic acid (1-3) is converted to an acyl hydrazide (1-4) by using the coupling reagent TFFH and hydrazine in the presence of a tertiary amine base such as triethylamine.
  • TFFH tertiary amine base
  • other coupling reagents commonly used for preparing amides may be used for this transformation along with hydrazine.
  • a bicyclo[2.2.2]octane-1-carboxylic ester can be heated with hydrazine to prepare acyl hydrazides (1-4).
  • acyl hydrazide (1-4) and iminoether (1-2) thus produced can be heated together in an inert high boiling organic solvent such as toluene in the presence of a tertiary amine base such as triethylamine to provide bicyclo[2.2.2]octyltriazoles (1-5) of structural formula I.
  • reaction can be conducted in the inverse manner as described by reaction Scheme 2.
  • a secondary amide (2-1) is prepared from a bicyclo[2.2.2]octane-1-carboxylic acid using a standard peptide coupling reaction.
  • This compound is methylated to form the iminoether (2-2) and reacted with an acyl hydrazide as described for reaction Scheme 1 to provide bicyclo[2.2.2]octyltriazoles (2-3) of structural formula I.
  • Reaction Scheme 3 describes an alternate approach to compounds of the present invention of structural formula I, in which the key step is the palladium catalyzed Suzuki coupling reaction between a bicyclo[2.2.2]octylbromotriazole (3-1) and an aryl boronic acid to produce triazoles (3-2) of structural formula I.
  • the preferred conditions use tetrakis(triphenylphosphine)palladium(0) as the catalyst in DMF solvent with cesium carbonate, but other catalysts and conditions may be employed, as recognized by those skilled in the art.
  • Reaction Scheme 4 describes yet another synthetic approach to the formation of compounds of structural formula I.
  • 4-(bicyclo[2.2.2]octyl)oxadiazoles (4-1) are dehydratively condensed with methylamine, either neat in a melt with methylammonium trifluoroacetate or in buffered MeOH solution. These reactions are best performed at high temperatures in a high pressure reactor to prevent the loss of methylamine.
  • Reaction Scheme 5 describes yet another synthetic approach to the formation of compounds of structural formula I.
  • bicyclo[2.2.2]octylcarboxamides (5-1) are converted to iminochlorides (5-2), using a reagent such as oxalyl chloride, thionyl chloride, phosphorus oxychloride or phosphorus pentachloride, optionally in the presence of DMF.
  • the iminochloride (5-2) is condensed with an aryl tetrazole in a high boiling inert organic solvent such as toluene to provide the triazole (5-3).
  • Intermediate Scheme 1 shows a preferred method for the preparation of oxadiazoles via the dehydration of diacyl hydrazides using a dehydrating reagent such as thionyl chloride.
  • a dehydrating reagent such as thionyl chloride.
  • other dehydrating reagents such as phosphorus oxychloride, phosphorus pentachloride or oxalyl chloride may be employed.
  • the diacyl hydrazides may be prepared preferentially from a hydrazide and an activated acid, such as an acid chloride, in the presence of a tertiary amine base.
  • standard peptide coupling reactions may be employed to prepare the diacyl hydrazide from a hydrazide and a carboxylic acid.
  • Intermediate Schemes 6 and 7 show preferred methods for the preparation of bicyclo[2.2.2]octane-1-carboxylic acids with a heteroaryl group at the R 3 position as given by structural formula I.
  • Oxadiazoles at the R 3 position may be prepared by the condensation of a bicyclo[2.2.2]octyl-1-carboxylic acid with an amidoxime as shown in Intermediate Scheme 6.
  • a useful reagent for this coupling is CDI.
  • other reagents useful for dehydration or peptide coupling reactions may be employed.
  • Intermediate Scheme 7 illustrates a preferred method for the synthesis of an intermediate of compounds of structural formula I bearing a thiazole group at the R 3 position.
  • Intermediate Schemes 8-14 show preferred methods for the preparation of bicyclo[2.2.2]octane-1-carboxylic acids intermediates in the synthesis of compounds of structural formula I with various alkyl or alkenyl or substituted alkyl groups at the R 3 position.
  • a key reaction is the Wittig reaction performed on a bicyclo[2.2.2]octane-1-carboxaldehyde, as shown in Intermediate Scheme 8.
  • the double bond in the product of this reaction may be hydrogenated to generate an alkyl group of varying length and character (which will become the R 3 substituent in structural formula I), depending on the Wittig reagent, as shown in Intermediate Scheme 9.
  • the double bond can be used to introduce other functionality, such as the hydroxy or fluoro group, as shown in Intermediate Scheme 10.
  • the aldehyde itself may be used to provide the difluoromethyl group at position R 3 , as shown in Intermediate Scheme 11.
  • the alkene product of the Wittig reaction can undergo numerous other transformations, for example, cyclopropanation, as illustrated in Intermediate Scheme 12.
  • the Wittig reagent may contain a remote functional group, for example, a ketal, as illustrated in Intermediate Scheme 13. This functional group may undergo characteristic functional group transformations after the Wittig/reduction sequence, for example, the hydrolysis of a ketal to a ketone, as illustrated in Intermediate Scheme 13, or the reduction of a ketal to an alcohol as illustrated in Intermediate Scheme 14.
  • compounds of structural formula I with a variety of different R 3 substituents may be obtained.
  • the specific examples given are intended to convey general principles and are not intended to limit the scope of the R 3 substituents.
  • Oxalyl chloride (3.49 ml, 40 mmol) was added dropwise to a solution of N-methyl-4-pentylbicyclo[2.2.2]octane-1-carboxamide (1-D) (952 mg, 4.0 mmol) in dry CH 2 Cl 2 at room temperature. After the vigorous gas evolution subsided, the solution was stirred at room temperature for 2 h. The CH 2 Cl 2 was removed carefully in vacuo at room temperature and then at 50°. The clear syrupy residue was dissolved in toluene (8 mL) and 5-[4-(benzyloxy)-2-methoxyphenyl]-2H-tetrazole (1-C) (1.13 g, 4.0 mmol) added.
  • the mixture was heated at 120° for 9 h.
  • the mixture was cooled, and the precipitated solid was filtered, washed with toluene and dried to afford the triazole hydrochloride salt.
  • the salt was partitioned between CH 2 Cl 2 and 10% aqueous K 2 CO 3 .
  • the aqueous phase was extracted twice with CH 2 Cl 2 .
  • the combined CH 2 Cl 2 extracts were dried (MgSO 4 ) and evaporated in vacuo.
  • Oxalyl chloride (505 ⁇ L, 5.79 mmol) was added dropwise to a mixture of 4-pentylbicyclo[2.2.2]octane-1-carboxylic acid (3-A) in methylene chloride (10 mL). The solution was stirred at room temperature for 3 h and then concentrated in vacuo to give 4-pentylbicyclo[2.2.2]octane-1-carbonyl chloride (3-B).
  • 1 H NMR 500 MHz, CDCl 3 ): ⁇ 0.90 (t, 3H); 1.21 (m, 8H); 1.45 (m, 6H); 1.88 (m, 6H) ppm.
  • N,N-Diisopropylethylamine (1.44 mL, 11.1 mmol) was added to a mixture of 4-pentylbicyclo[2.2.2]octane-1-carboxylic acid (3-A) (1.09 g, 4.45 mmol) and methylamine hydrochloride (1.5 g, 22.3 mmol) in methylene chloride (10 mL) was added and the mixture stirred at room temperature for 18 h. After diluting with methylene chloride, the mixture was washed with water, brine, dried (MgSO 4 ) and concentrated in vacuo to give N-methyl-4-pentylbicyclo[2.2.2]octane-1-carboxamide (3-C).
  • 1 H NMR 500 MHz, CDCl 3 ): ⁇ 0.91 (t, 3H); 1.22 (m, 8H); 1.43 (m, 6H); 1.77 (m, 6H); 2.82 (d, 3H) ppm.
  • Oxalyl chloride (846 ⁇ L, 9.7 mmol) was added dropwise to a solution of N-methyl-4-pentylbicyclo[2.2.2]octane-1-carboxamide (3-C) (230 mg, 0.97 mmol) in methylene chloride (2.0 mL) and the mixture stirred at room temperature for 4 h. The solvent and excess reagent were removed in vacuo to provide N-methyl-4-pentylbicyclo[2.2.2]octane-1-carboximidoyl chloride (3-D).
  • the ester (7-B) (1.01 g, 3.06 mmol) was treated with KOH (0.52 g, 9.18 mmol) in methanol/water (95/5, 20 mL). After it was heated at 60° C. for 12 h, the reaction mixture was concentrated, diluted with water, extracted twice with ethyl acetate. The aqueous layer was acidified with 1N HC1 aqueous solution and a white solid precipitated out. The solid 4-[3-(4-fluorophenyl)-1,2,4-oxadiazol-5-yl]bicyclo[2.2.2]octane-1-carboxylic acid (7-C) was collected and further dried by co-evaporating with toluene. ESI-MS m/z (M+H) 317.2.
  • the trifluoroacetate salt of methylamine (380 mg, 2.61 mmol) and 2-[4-(benzyloxy)-2-(trifluoromethyl)phenyl]-5-(4-phenylbicyclo[2.2.2]oct-1-yl)-1,3,4-oxadiazole (8-D) were suspended in a 2 M solution of methylamine in methanol (1.3 mL, 2.61 mmol) and heated at 150° C. overnight. After being cooled to room temperature, the reaction mixture was partitioned between ethyl acetate (25 mL) and saturated aqueous sodium bicarbonate (30 mL).
  • Triazole 9-D (30 mg, 0.08 mmol) was dissolved in 0.5 mL of dry methylene chloride, placed under an inert atmosphere, and cooled to 0° C. To this solution was added BBr 3 (1 M in CH 2 Cl 2 , 0.25 mL, 0.25 mmol) and the cooling bath was immediately removed. The reaction was stirred for 2 h then diluted with 20 mL of methylene chloride and washed with 1 N aqueous NaOH and brine. The residue was chromatographed by reverse-phase HPLC, eluting with a gradient of 0 to 100% acetonitrile in water.
  • Ester 10-3 (880 mg, 3 mmol) was dissolved in 10% water/methanol solution (100 mL) and treated with 1 g of potassium hydroxide. The reaction was heated at 60° C. for 1 h then at 45° C. overnight. The mixture was concentrated in vacuo then acidified to pH 2 with 1M HCl and extracted with three portions of methylene chloride. The organic layers were combined, dried over anhydrous sodium sulfate and evaporated to give 4-[2-(ethylsulfonyl)ethyl]bicyclo[2.2.2]octane-1-carboxylic acid (10-4).
  • Carboxylic acid 10-4 (810 mg, 2.96 mmol) was dissolved in 12 mL of anhydrous methylene chloride under nitrogen atmosphere, treated with oxalyl chloride (2M in methylene chloride, 4.4 mL, 8.8 mmol) and subsequently with 5 drops of DMF. The reaction was stirred at room temperature under nitrogen atmosphere for 90 min, then evaporated and placed under vacuum for 20 min. The acid chloride was dissolved in anhydrous methylene chloride (12 mL), cooled in an ice-bath, and then treated dropwise with a solution of methylamine (2M in THF, 8.9 mL, 17.8 mmol). Upon addition of the amine, the cooling bath was removed and the reaction stirred at ambient temperature for 30 min.
  • Methyl amide 10-5 (220 mg, 0.77 mmol) was dissolved in anhydrous methylene chloride (2 mL) and treated with oxalyl chloride (2M in methylene chloride, 0.77 mL, 1.54 mmol) and DMF (2 drops). The solution was stirred at room temperature for 1 h, then solvent removed by evaporation under diminished pressure. The residue was redissolved in anhydrous toluene (2 mL) and treated with 5 [2-(trifluoromethyl)phenyl]1H-tetrazole (214 mg, 1 mmol). The mixture was refluxed for 18 h.
  • the reaction was cooled to room temperature and the cream-colored precipitate was filtered and washed to give 300 mg of crude product as the HCl salt.
  • the salt was taken up in methylene chloride/1N HCl and the aqueous layer was washed with two additional portions of methylene chloride.
  • the organic layers were combined and evaporated and the residue was chromatographed by flash silica gel chromatography. Elution was carried out with a gradient ranging from 0 to 5% methanol/methylene chloride.
  • Diester 11-2 (0.625 g, 1.90 mmol) was dissolved in a 1:1 mixture of ethyl acetate/methanol (30 mL), placed under nitrogen atmosphere, then treated with 10% Pd/C (500 mg) and 0.1 mL of acetic acid. The reaction was placed under hydrogen atmosphere and stirred vigorously for 2 hr. The resulting solution was filtered through celite and the solvent was removed under reduced pressure. The residue was partitioned between 200 mL of ethyl acetate and 200 mL of 1 N NaOH solution. The aqueous layer was separated and neutralized, then extracted three times with 50 mL of methylene chloride.
  • Carboxylic acid 11-3 (400 mg, 1.67 mmol) was dissolved in tetrahydrofuran (5 mL) and borane (1 M solution in THF, 2.17 mL, 1.3 eq.) was added dropwise at room temperature. After 2 h the reaction was added to 50 mL of 1 N HCl and then extracted three times with 50 mL of methylene chloride. The combined organic layers were dried over magnesium sulfate and the solvent was removed under reduced pressure to afford crude methyl 4-(3-hydroxypropyl)bicyclo [2.2.2]octane-1-carboxylate (11-4) which was used without purification in the next step.
  • Hydroxyester 11-4 (430 mg, 1.9 mmol) was dissolved in 2.5 mL of anhydrous methylene chloride under nitrogen atmosphere, treated with pyridine (0.5 mL) and methanesulfonyl chloride (0.368 mL, 4.8 mmol) and stirred for 4 h at room temperature. The mixture was diluted with 100 mL of ethyl acetate and washed with 1N aqueous HC1, saturated aqueous sodium bicarbonate, and brine. The organic layer was dried over anhydrous sodium sulfate and evaporated.
  • Sulfide 11-6 (3.0 g, 11 mmol) was dissolved in methylene chloride (50 mL) and treated with m-chloroperbenzoic acid (75%, 6.2 g). The solution was stirred at room temperature for 2 h, then the mixture was diluted with 100 mL of methylene chloride and washed with saturated aqueous sodium bicarbonate, then twice with saturated aqueous sodium bisulfite, then twice with saturated aqueous sodium bicarbonate, and brine.
  • Carboxylic acid 11-8 (3.0 g, 11 mmol) was dissolved in 50 mL of anhydrous methylene chloride under nitrogen atmosphere, treated with oxalyl chloride (2 M in methylene chloride, 16.2 mL, 32.4 mmol) and subsequently with 5 drops of DMF. The reaction was stirred at room temperature under nitrogen atmosphere for 90 min, then evaporated and placed under vacuum for 20 min. The acid chloride was dissolved in anhydrous methylene chloride (12 mL), cooled in an ice-bath, and then treated dropwise with a solution of methylamine (2M in THF, 27 mL, 54 mmol). Upon addition of the methylamine, the cooling bath was removed and the reaction stirred at ambient temperature for 30 min.
  • Methyl amide 11-9 (0.470 g, 1.56 mmol) was dissolved in anhydrous methylene chloride (5 mL) and treated with oxalyl chloride (2M in methylene chloride, 1.56 mL, 3.12 mmol) and DMF (2 drops). The solution was stirred at room temperature for 1 h, then solvent removed by evaporation under reduced pressure. The residue was redissolved in anhydrous toluene (7 mL) and treated with 5 [2-(trifluoromethyl)phenyl]1H-tetrazole (368 mg, 1.72 mmol). The mixture was refluxed for 18 h.
  • the reaction was cooled to room temperature and the precipitate was filtered and washed to give 300 mg of crude product as the HCl salt.
  • the salt was taken up in methylene chloride/1N HCl and the aqueous layer was washed with two additional portions of methylene chloride.
  • the organic layers were combined and evaporated and the residue was chromatographed by flash silica gel chromatography. Elution was carried out with a gradient ranging from 0 to 5% methanol/methylene chloride.
  • the reaction mixture was stirred overnight under nitrogen atmosphere at ambient temperature followed by addition of another portion of methanesulfonyl fluoride (4.05 ml, 58.9 mmol) and aluminum trichloride (9.17 g, 68.8 mmol).
  • the resulting mixture was heated at 80° C. for 3 h, then cooled to room temperature and diluted with 300 ml of dichloromethane and 200 ml water. The layers were separated and the aqueous layer was washed with two 100 ml portions of dichloromethane. The organic layers were combined, washed with brine, dried (MgSO 4 ), and concentrated in vacuo.
  • Carboxylic acid 12-C was prepared in quantitative yield by hydrolysis of ester 12-B (1.1 g, 3.4 mmol) using the procedures described in Example 11, Step G.
  • Carboxylic acid 12-C (0.99 g, 3.2 mmol) was converted to hydrazide 12-D using hydrazine (0.124 ml, 4 mmol) and the standard coupling procedure analogous to Example 9, step A.
  • Crude product was purified by flash silica gel chromatography eluting with 0-2% MeOH/CH 2 Cl 2 gradient to yield a white powder.
  • MS (ESI + ) 323.2 (M+1).
  • Triazole 14-B was prepared from nitrile 13-E (0.053 g, 0.14 mmol) and 3,3,3-trifluoromethylpropionic acid (0.036 ml, 0.41 mmol) using the method described in Example 13, step E. 3-(4- ⁇ 4-Methyl-5-[2-(trifluoromethyl)phenyl]-4H-1,2,4-triazol-3-yl ⁇ bicyclo [2.2.2]oct-1-yl)-5-(3,3,3-trifluoroethyl)-1,2,4-oxadiazole (14-B) was isolated as a white powder.
  • Methyl amide 15-F (0.030 g, 0.092 mmol) was converted to triazole 15-G using the procedures outlined in Example 10, step E.
  • 4-Methyl-3-[2-(trifluoromethyl)phenyl]-5-(4- ⁇ 2-[(trifluoromethyl)sulfonyl]ethyl ⁇ bicyclo[2.2.2]oct-1-yl)-4H-1,2,4-triazole (15-G) was isolated as a white powder; MS (ESI + ) 496.4 (M+1).
  • an oral composition of a compound of the present invention 50 mg of any of Examples 1-15 is formulated with sufficient finely divided lactose to provide a total amount of 580 to 590 mg to fill a size O hard gelatin capsule.

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Abstract

Triazole derivatives of structural formula I are selective inhibitors of the 11β-hydroxysteroid dehydrogenase-1. The compounds are useful for the treatment of diabetes, such as noninsulin-dependent diabetes (NIDDM), hyperglycemia, obesity, insulin resistance, dyslipidemia, hyperlipidemia, hypertension, Metabolic Syndrome, and other symptoms associated with NIDDM.

Description

    FIELD OF THE INVENTION
  • The present invention relates to triazole derivatives as inhibitors of the enzyme 11-beta-hydroxysteroid dehydrogenase Type I (11β-HSD-1 or HSD-1) and methods of treatment certain conditions using such compounds. The compounds of the present invention are useful for the treatment of diabetes, such as non-insulin dependent Type 2 diabetes mellitus (NIDDM), insulin resistance, obesity, lipid disorders, hypertension, and other diseases and conditions.
    • BACKGROUND OF THE INVENTION
  • Diabetes is caused by multiple factors and is most simply characterized by elevated levels of plasma glucose (hyperglycemia) in the fasting state. There are two generally recognized forms of diabetes: Type 1 diabetes, or insulin-dependent diabetes mellitus (IDDM), in which patients produce little or no insulin, the hormone which regulates glucose utilization, and Type 2 diabetes, or noninsulin-dependent diabetes mellitus (NIDDM), wherein patients produce insulin and even exhibit hyperinsulinemia (plasma insulin levels that are the same or even elevated in comparison with non-diabetic subjects), while at the same time demonstrating hyperglycemia. Type 1 diabetes is typically treated with exogenous insulin administered via injection. However, Type 2 diabetics often develop “insulin resistance”, such that the effect of insulin in stimulating glucose and lipid metabolism in the main insulin-sensitive tissues, namely, muscle, liver and adipose tissues, is diminished. Patients who are insulin resistant but not diabetic have elevated insulin levels that compensate for their insulin resistance, so that serum glucose levels are not elevated. In patients with NIDDM, the plasma insulin levels, even when they are elevated, are insufficient to overcome the pronounced insulin resistance, resulting in hyperglycemia.
  • Insulin resistance is primarily due to a receptor binding defect that is not yet completely understood. Resistance to insulin results in insufficient activation of glucose uptake, diminished oxidation of glucose and storage of glycogen in muscle, inadequate insulin repression of lipolysis in adipose tissue and inadequate glucose production and secretion by the liver.
  • Persistent or uncontrolled hyperglycemia that occurs in diabetics is associated with increased morbidity and premature mortality. Abnormal glucose homeostasis is also associated both directly and indirectly with obesity, hypertension and alterations in lipid, lipoprotein and apolipoprotein metabolism. Type 2 diabetics are at increased risk of developing cardiovascular complications, e.g., atherosclerosis, coronary heart disease, stroke, peripheral vascular disease, hypertension, nephropathy, neuropathy and retinopathy. Therefore, therapeutic control of glucose homeostasis, lipid metabolism, obesity and hypertension are critically important in the clinical management and treatment of diabetes mellitus.
  • Many patients who have insulin resistance but have not developed Type 2 diabetes are also at a risk of developing symptoms referred to as “Syndrome X” or “Metabolic Syndrome”. Syndrome X or Metabolic Syndrome is characterized by insulin resistance, along with abdominal obesity, hyperinsulinemia, high blood pressure, low HDL and high VLDL. These patients, whether or not they develop overt diabetes mellitus, are at increased risk of developing the cardiovascular complications listed above.
  • Treatment of Type 2 diabetes typically includes physical exercise and dieting. Increasing the plasma level of insulin by administration of sulfonylureas (e.g. tolbutamide and glipizide) or meglitinide, which stimulate the pancreatic β-cells to secrete more insulin, and/or by injection of insulin when sulfonylureas or meglitinide become ineffective, can result in insulin concentrations high enough to stimulate insulin-resistant tissues. However, dangerously low levels of plasma glucose can result, and an increased level of insulin resistance can ultimately occur.
  • Biguanides increase insulin sensitivity, resulting in some correction of hyperglycemia. However, many biguanides, e.g., phenformin and metformin, cause lactic acidosis, nausea and diarrhea.
  • The glitazones (i.e. 5-benzylthiazolidine-2,4-diones) form a newer class of compounds with the potential for ameliorating hyperglycemia and other symptoms of Type 2 diabetes. These agents substantially increase insulin sensitivity in muscle, liver and adipose tissue, resulting in partial or complete correction of the elevated plasma levels of glucose substantially without causing hypoglycemia. The glitazones that are currently marketed are agonists of the peroxisome proliferator activated receptor (PPAR) gamma subtype. PPAR-gamma agonism is generally believed to be responsible for the improved insulin sensitization that is observed with the glitazones. Newer PPAR agonists that are being developed for treatment of Type 2 diabetes and/or dyslipidemia are agonists of one or more of the PPAR alpha, gamma and delta subtypes. For a review of insulin-sensitizing agents and other mechanisms for the treatment of Type 2 diabetes, see M. Tadayyon and S. A. Smith, “Insulin sensitisation in the treatment of Type 2 diabetes,” Expert Opin. Investig. Drugs, 12: 307-324 (2003).
  • There is a continuing need for new methods of treating diabetes and related conditions, such as Metabolic Syndrome. The present invention meets this and other needs.
    • SUMMARY OF THE INVENTION
  • The present invention relates to bicyclo[2.2.2]-oct-1-yl-1,2,4-triazoles of structural formula I
  • Figure US20090181994A1-20090716-C00001
  • These bicyclo[2.2.2]-octyltriazole derivatives are effective as inhibitors of 11β-hydroxysteroid dehydrogenase type 1 (11β-HSD1). They are therefore useful for the treatment, control or prevention of disorders responsive to the inhibition of 11α-HSD1, such as Type 2 diabetes, lipid disorders, obesity, atherosclerosis, and Metabolic Syndrome.
  • The present invention also relates to pharmaceutical compositions comprising the compounds of the present invention and a pharmaceutically acceptable carrier.
  • The present invention also relates to methods for the treatment, control, or prevention of disorders, diseases, or conditions responsive to inhibition of 11β-HSD1 in a subject in need thereof by administering the compounds and pharmaceutical compositions of the present invention.
  • The present invention also relates to methods for the treatment or control of Type 2 diabetes, obesity, lipid disorders, atherosclerosis, and Metabolic Syndrome by administering the compounds and pharmaceutical compositions of the present invention.
  • The present invention also relates to methods for treating obesity by administering the compounds of the present invention in combination with a therapeutically effective amount of another agent known to be useful to treat the condition.
  • The present invention also relates to methods for treating Type 2 diabetes by administering the compounds of the present invention in combination with a therapeutically effective amount of another agent known to be useful to treat the condition.
  • The present invention also relates to methods for treating atherosclerosis by administering the compounds of the present invention in combination with a therapeutically effective amount of another agent known to be useful to treat the condition.
  • The present invention also relates to methods for treating lipid disorders by administering the compounds of the present invention in combination with a therapeutically effective amount of another agent known to be useful to treat the condition.
  • The present invention also relates to methods for treating Metabolic Syndrome by administering the compounds of the present invention in combination with a therapeutically effective amount of another agent known to be useful to treat the condition.
  • The present invention is also concerned with the use of the compounds of structural formula I for the treatment hyperglycemia, insulin resistance, Type 2 diabetes, lipid disorders, obesity, atherosclerosis, and Metabolic Syndrome.
  • The present invention also provides for the use of the compounds of structural formula I in the manufacture of a medicament for use in the treatment of hyperglycemia, insulin resistance, Type 2 diabetes, lipid disorders, obesity, atherosclerosis, and Metabolic Syndrome.
    • DETAILED DESCRIPTION OF THE INVENTION
  • The present invention is concerned with bicyclo[2.2.2]-oct-1-yl-1,2,4-triazole derivatives useful as inhibitors of 11β-HSD1. Compounds of the present invention are described by structural formula I:
  • Figure US20090181994A1-20090716-C00002
  • or a pharmaceutically acceptable salt thereof; wherein
    each p is independently 0, 1, or 2;
    each n is independently 0, 1, or 2;
    X is selected from the group consisting of a single bond, O, S(O)p, NR6,
  • Figure US20090181994A1-20090716-C00003
  • R1 is selected from the group consisting of
  • arylcarbonyl,
  • (CH2)n-aryl, and
  • (CH2)n-heteroaryl;
  • in which aryl and heteroaryl are unsubstituted or substituted with one to three substituents independently selected from R5;
    R2 is selected from the group consisting of
  • hydrogen,
  • C1-8 alkyl,
  • C2-6 alkenyl, and
  • (CH2)n—C3-6 cycloalkyl,
  • in which alkyl, alkenyl, and cycloalkyl are unsubstituted or substituted with one to three substituents independently selected from R8 and oxo;
    each R4 is independently selected from the group consisting of
  • hydrogen,
  • halogen,
  • hydroxy,
  • oxo,
  • C1-3 alkyl, and
  • C1-3 alkoxy;
  • R3 is selected from the group consisting of
  • hydrogen,
  • C1-10 alkyl,
  • C2-10 alkenyl,
  • (CH2)n—C3-6 cycloalkyl,
  • (CH2)n-aryl,
  • (CH2)n-heteroaryl, and
  • (CH2)n-heterocyclyl;
  • in which aryl, heteroaryl, and heterocyclyl are unsubstituted or substituted with one to three substituents independently selected from R5; and alkyl, alkenyl, and cycloalkyl are unsubstituted or substituted with one to five groups independently selected from R8 and oxo;
    R5 and R8 are each independently selected from the group consisting of
  • hydrogen,
  • formyl,
  • C1-6 alkyl,
  • (CH2)n-aryl,
  • (CH2)n-heteroaryl,
  • (CH2)n-heterocyclyl,
  • (CH2)nC3-7 cycloalkyl,
  • halogen,
  • OR7,
  • (CH2)nN(R7)2,
  • cyano,
  • (CH2)nCO2R7,
  • NO2,
  • (CH2)nNR7SO2R6,
  • (CH2)nSO2N(R7)2,
  • (CH2)nS(O)pR6,
  • (CH2)nSO20R7,
  • (CH2)nNR7C(O)N(R7)2,
  • (CH2)nC(O)N(R7)2,
  • (CH2)nNR6C(O)R6,
  • (CH2)nNR6CO2R7,
  • O(CH2)nC(O)N(R7)2,
  • CF3,
  • CH2CF3,
  • OCF3,
  • OCHCF2, and
  • OCH2CF3;
  • wherein aryl, heteroaryl, cycloalkyl, and heterocyclyl are unsubstituted or substituted with one to three substituents independently selected from halogen, hydroxy, C1-4 alkyl, trifluoromethyl, trifluoromethoxy, and C1-4 alkoxy; and wherein any methylene (CH2) carbon atom in R5 and R8 is unsubstituted or substituted with one to two groups independently selected from halogen, hydroxy, and C1-4 alkyl; or two substituents when on the same methylene (CH2) carbon atom are taken together with the carbon atom to which they are attached to form a cyclopropyl group;
    each R6 is independently selected from the group consisting of
  • C1-8 alkyl,
  • (CH2)n-aryl,
  • (CH2)n-heteroaryl, and
  • (CH2)nC3-7 cycloalkyl;
  • wherein alkyl and cycloalkyl are unsubstituted or substituted with one to five substituents independently selected from halogen, oxo, C1-4 alkoxy, C1-4 alkylthio, hydroxy, amino; and aryl and heteroaryl are unsubstituted or substituted with one to three substituents independently selected from cyano, halogen, hydroxy, amino, carboxy, trifluoromethyl, trifluoromethoxy, C1-4 alkyl, and C1-4 alkoxy; or two R6 groups together with the atom to which they are attached form a 5- to 8-membered mono- or bicyclic ring system optionally containing an additional heteroatom selected from O, S, and NC1-4 alkyl; and
    each R7 is hydrogen or R6.
  • In one embodiment of the compounds of the present invention, R2 is cyclopropyl, C1-3 alkyl, or C2-3 alkenyl and R1 is phenyl or naphthyl in which phenyl and naphthyl are unsubstituted or substituted with one to three substituents independently selected from R5. In a class of this embodiment, R5 is selected from the group consisting of halogen, hydroxy, trifluoromethyl, trifluoromethoxy, C1-3 alkyl, C1-3 alkoxy, C1-3 alkylthio, and C1-3 alkylsulfonyl. In a subclass of this class, R2 is methyl and R4 is hydrogen.
  • In a second embodiment of the compounds of the present invention,
  • X is a single bond;
    R1 is phenyl or naphthyl in which phenyl and naphthyl are unsubstituted or substituted with one to three substituents independently selected from R5;
    R2 is cyclopropyl, C1-3 alkyl, or C2-3 alkenyl; and
    R3 is C1-6 alkyl unsubstituted or substituted with one to three substituents independently selected from R8 and oxo.
  • In a class of this second embodiment, R5 is selected from the group consisting of halogen, hydroxy, trifluoromethyl, trifluoromethoxy, C1-3 alkyl, C1-3 alkoxy, C1-3 alkylthio, and C1-3 alkylsulfonyl. In a subclass of this class, R2 is methyl and R4 is hydrogen. In another class of this embodiment, R8 is selected from the group consisting of halogen, hydroxy, oxo, C1-4 alkoxy, C1-4 alkylthio, C1-4 alkylsulfinyl, C1-4 alkylsulfonyl, and phenyl unsubstituted or substituted with one to three groups independently selected from halogen and trifluoromethyl. In a subclass of this class, R2 is methyl and R4 is hydrogen. In a third class of this embodiment, R5 is selected from the group consisting of halogen, hydroxy, trifluoromethyl, trifluoromethoxy, C1-3 alkyl, C1-3 alkoxy, C1-3 alkylthio, and C1-3 alkylsulfonyl; and R8 is selected from the group consisting of halogen, hydroxy, oxo, C1-4 alkoxy, C1-4 alkylthio, C1-4 alkylsulfonyl, and phenyl unsubstituted or substituted with one to three groups independently selected from halogen and trifluoromethyl. In a subclass of this class, R2 is methyl and R4 is hydrogen.
  • In a third embodiment of the compounds of the present invention,
  • X is a single bond;
    R1 is phenyl or naphthyl in which phenyl and naphthyl are unsubstituted or substituted with one to three substituents independently selected from R5;
    R2 is cyclopropyl, C1-3 alkyl, or C2-3 alkenyl; and
    R3 is phenyl or heteroaryl wherein phenyl and heteroaryl are unsubstituted or substituted with one with one to three substituents independently selected from R5.
  • In a class of this embodiment, R2 is methyl and R4 is hydrogen.
  • In another class of this embodiment, R3 is phenyl unsubstituted or substituted with one with one to three substituents independently selected from R5. In a subclass of this class, R5 is selected from the group consisting of halogen, hydroxy, trifluoromethyl, trifluoromethoxy, C1-3 alkyl, C1-3 alkoxy, C1-3 alkylthio, and C1-3 alkylsulfonyl. In a subclass of this subclass, R2 is methyl and R4 is hydrogen.
  • In a third class of this embodiment, R3 is oxadiazolyl, unsubstituted or substituted with one with one to two substituents independently selected from R5. In a subclass of this class, R5 is phenyl unsubstituted or substituted with one to three substituents independently selected from halogen, hydroxy, C1-4 alkyl, trifluoromethyl, trifluoromethoxy, and C1-4 alkoxy. In a subclass of this subclass, R2 is methyl and R4 is hydrogen.
  • Illustrative, but nonlimiting examples, of compounds of the present invention that are useful as inhibitors of 11-beta-hydroxysteroid dehydrogenase Type I are the following:
  • Figure US20090181994A1-20090716-C00004
    Figure US20090181994A1-20090716-C00005
    Figure US20090181994A1-20090716-C00006
  • or a pharmaceutically acceptable salt thereof.
  • As used herein the following definitions are applicable.
  • “Alkyl”, as well as other groups having the prefix “alk”, such as alkoxy and alkanoyl, means carbon chains which may be linear or branched, and combinations thereof, unless the carbon chain is defined otherwise. Examples of alkyl groups include methyl, ethyl, propyl, isopropyl, butyl, sec- and tert-butyl, pentyl, hexyl, heptyl, octyl, nonyl, and the like. Where the specified number of carbon atoms permits, e.g., from C3-10, the term alkyl also includes cycloalkyl groups, and combinations of linear or branched alkyl chains combined with cycloalkyl structures. When no number of carbon atoms is specified, C1-6 is intended.
  • “Alkenyl” means carbon chains which contain at least one carbon-carbon double bond, and which may be linear or branched or combinations thereof, unless the carbon chain is defined otherwise. Examples of alkenyl include vinyl, allyl, isopropenyl, pentenyl, hexenyl, heptenyl, 1-propenyl, 2-butenyl, 2-methyl-2-butenyl, and the like. Where the specified number of carbon atoms permits, e.g., from C5-10, the term alkenyl also includes cycloalkenyl groups, and combinations of linear, branched and cyclic structures. When no number of carbon atoms is specified, C2-6 is intended.
  • “Alkynyl” means carbon chains which contain at least one carbon-carbon triple bond, and which may be linear or branched or combinations thereof. Examples of alkynyl include ethynyl, propargyl, 3-methyl-1-pentynyl, 2-heptynyl, and the like.
  • “Cycloalkyl” is a subset of alkyl and means a saturated carbocyclic ring having a specified number of carbon atoms. Examples of cycloalkyl include cyclopropyl, cyclobutyl, cyclopentyl, cyclohexyl, cycloheptyl, cyclooctyl, and the like. A cycloalkyl group generally is monocyclic unless stated otherwise. Cycloalkyl groups are saturated unless otherwise defined.
  • The term “alkoxy” refers to straight or branched chain alkoxides of the number of carbon atoms specified (e.g., C1-6 alkoxy), or any number within this range [i.e., methoxy (MeO—), ethoxy, isopropoxy, etc.].
  • The term “alkylthio” refers to straight or branched chain alkylsulfides of the number of carbon atoms specified (e.g., C1-6 alkylthio), or any number within this range [i.e., methylthio (MeS—), ethylthio, isopropylthio, etc.].
  • The term “alkylamino” refers to straight or branched alkylamines of the number of carbon atoms specified (e.g., C1-6 alkylamino), or any number within this range [i.e., methylamino, ethylamino, isopropylamino, t-butylamino, etc.].
  • The term “alkylsulfonyl” refers to straight or branched chain alkylsulfones of the number of carbon atoms specified (e.g., C1-6 alkylsulfonyl), or any number within this range [i.e., methylsulfonyl (MeSO2—), ethylsulfonyl, isopropylsulfonyl, etc.].
  • The term “alkylsulfinyl” refers to straight or branched chain alkylsulfoxides of the number of carbon atoms specified (e.g., C1-6 alkylsulfinyl), or any number within this range [i.e., methylsulfinyl (MeSO—), ethylsulfinyl, isopropylsulfinyl, etc.].
  • The term “alkyloxycarbonyl” refers to straight or branched chain esters of a carboxylic acid derivative of the present invention of the number of carbon atoms specified (e.g., C1-6 alkyloxycarbonyl), or any number within this range [i.e., methyloxycarbonyl (MeOCO—), ethyloxycarbonyl, or butyloxycarbonyl].
  • “Aryl” means a mono- or polycyclic aromatic ring system containing carbon ring atoms. The preferred aryls are monocyclic or bicyclic 6-10 membered aromatic ring systems. Phenyl and naphthyl are preferred aryls. The most preferred aryl is phenyl.
  • “Heterocycle” and “heterocyclyl” refer to saturated or unsaturated non-aromatic rings or ring systems containing at least one heteroatom selected from O, S and N, further including the oxidized forms of sulfur, namely SO and SO2. Examples of heterocycles include tetrahydrofuran (THF), dihydrofuran, 1,4-dioxane, morpholine, 1,4-dithiane, piperazine, piperidine, 1,3-dioxolane, imidazolidine, imidazoline, pyrroline, pyrrolidine, tetrahydropyran, dihydropyran, oxathiolane, dithiolane, 1,3-dioxane, 1,3-dithiane, oxathiane, thiomorpholine, and the like.
  • “Heteroaryl” means an aromatic or partially aromatic heterocycle that contains at least one ring heteroatom selected from O, S and N. Heteroaryls thus includes heteroaryls fused to other kinds of rings, such as aryls, cycloalkyls and heterocycles that are not aromatic. Examples of heteroaryl groups include: pyrrolyl, isoxazolyl, isothiazolyl, pyrazolyl, pyridyl, oxazolyl, oxadiazolyl, thiadiazolyl, thiazolyl, imidazolyl, triazolyl, tetrazolyl, furyl, triazinyl, thienyl, pyrimidyl, benzisoxazolyl, benzoxazolyl, benzothiazolyl, benzothiadiazolyl, dihydrobenzofuranyl, indolinyl, pyridazinyl, indazolyl, isoindolyl, dihydrobenzothienyl, indolizinyl, cinnolinyl, phthalazinyl, quinazolinyl, naphthyridinyl, carbazolyl, benzodioxolyl, quinoxalinyl, purinyl, furazanyl, isobenzylfuranyl, benzimidazolyl, benzofuranyl, benzothienyl, quinolyl, indolyl, isoquinolyl, dibenzofuranyl, and the like. For heterocyclyl and heteroaryl groups, rings and ring systems containing from 3-15 atoms are included, forming 1-3 rings.
  • “Halogen” refers to fluorine, chlorine, bromine and iodine. Chlorine and fluorine are generally preferred. Fluorine is most preferred when the halogens are substituted on an alkyl or alkoxy group (e.g. CF3O and CF3CH2O).
  • The term “composition”, as in pharmaceutical composition, is intended to encompass a product comprising the active ingredient(s), and the inert ingredient(s) that make up the carrier, as well as any product which results, directly or indirectly, from combination, complexation or aggregation of any two or more of the ingredients, or from dissociation of one or more of the ingredients, or from other types of reactions or interactions of one or more of the ingredients. Accordingly, the pharmaceutical compositions of the present invention encompass any composition made by admixing a compound of the present invention and a pharmaceutically acceptable carrier.
  • The terms “administration of” and “administering a” compound should be understood to mean providing a compound of the invention or a prodrug of a compound of the invention to the individual in need.
  • Compounds of structural formula I may contain one or more asymmetric centers and can thus occur as racemates and racemic mixtures, single enantiomers, diastereomeric mixtures and individual diastereomers. The present invention is meant to comprehend all such isomeric forms of the compounds of structural formula I.
  • Some of the compounds described herein contain olefinic double bonds, and unless specified otherwise, are meant to include both E and Z geometric isomers.
  • Some of the compounds described herein may exist as tautomers such as keto-enol tautomers. The individual tautomers, as well as mixtures thereof, are encompassed within the compounds of structural formula I.
  • Compounds of structural formula I may be separated into their individual diastereoisomers by, for example, fractional crystallization from a suitable solvent, for example methanol or ethyl acetate or a mixture thereof, or via chiral chromatography using an optically active stationary phase. Absolute stereochemistry may be determined by X-ray crystallography of crystalline products or crystalline intermediates which are derivatized, if necessary, with a reagent containing an asymmetric center of known absolute configuration.
  • Alternatively, any stereoisomer of a compound of the general structural formula I may be obtained by stereospecific synthesis using optically pure starting materials or reagents of known absolute configuration.
  • In a different aspect of the invention, a pharmaceutical composition is addressed comprising a compound in accordance with structural formula I, or a pharmaceutically acceptable salt or solvate thereof, in combination with a pharmaceutically acceptable carrier. By the term “solvate” is meant a hydrate, an alcoholate, or other solvate of crystallization.
  • In another aspect of the invention, a method of treating hyperglycemia, diabetes or insulin resistance in a mammalian patient in need of such treatment is addressed, which comprises administering to said patient an effective amount of a compound in accordance with structural formula I or a pharmaceutically salt or solvate thereof.
  • In another aspect of the invention, a method of treating non-insulin dependent (Type 2) diabetes mellitus in a mammalian patient in need of such treatment is disclosed comprising administering to the patient an anti-diabetic effective amount of a compound in accordance with structural formula I.
  • In another aspect of the invention, a method of treating obesity in a mammalian patient in need of such treatment is disclosed comprising administering to said patient a compound in accordance with structural formula I in an amount that is effective to treat obesity.
  • In another aspect of the invention, a method of treating Metabolic Syndrome in a mammalian patient in need of such treatment is disclosed, comprising administering to said patient a compound in accordance with structural formula I in an amount that is effective to treat Metabolic Syndrome.
  • In another aspect of the invention, a method of treating a lipid disorder selected from the group consisting of dyslipidemia, hyperlipidemia, hypertriglyceridemia, hypercholesterolemia, low HDL, and high LDL in a mammalian patient in need of such treatment is disclosed, comprising administering to said patient a compound in accordance with structural formula I in an amount that is effective to treat said lipid disorder.
  • In another aspect of the invention, a method of treating atherosclerosis in a mammalian patient in need of such treatment is disclosed, comprising administering to said patient a compound in accordance with structural formula I in an amount effective to treat atherosclerosis.
  • In another aspect of the invention, a method of treating a condition selected from the group consisting of: (1) hyperglycemia, (2) low glucose tolerance, (3) insulin resistance, (4) obesity, (5) lipid disorders, (6) dyslipidemia, (7) hyperlipidemia, (8) hypertriglyceridemia, (9) hypercholesterolemia, (10) low HDL levels, (11) high LDL levels, (12) atherosclerosis and its sequelae, (13) vascular restenosis, (14) pancreatitis, (15) abdominal obesity, (16) neurodegenerative disease, (17) retinopathy, (18) nephropathy, (19) neuropathy, (20) Metabolic Syndrome, (21) hypertension and other conditions and disorders where insulin resistance is a component, in a mammalian patient in need of such treatment is disclosed, comprising administering to the patient a compound in accordance with structural formula I in an amount that is effective to treat said condition.
  • In another aspect of the invention, a method of delaying the onset of a condition selected from the group consisting of (1) hyperglycemia, (2) low glucose tolerance, (3) insulin resistance, (4) obesity, (5) lipid disorders, (6) dyslipidemia, (7) hyperlipidemia, (8) hypertriglyceridemia, (9) hypercholesterolemia, (10) low HDL levels, (11) high LDL levels, (12) atherosclerosis and its sequelae, (13) vascular restenosis, (14) pancreatitis, (15) abdominal obesity, (16) neurodegenerative disease, (17) retinopathy, (18) nephropathy, (19) neuropathy, (20) Metabolic Syndrome, (21) hypertension and other conditions and disorders where insulin resistance is a component in a mammalian patient in need of such treatment is disclosed, comprising administering to the patient a compound in accordance with structural formula I in an amount that is effective to delay the onset of said condition.
  • In another aspect of the invention, a method of reducing the risk of developing a condition selected from the group consisting of (1) hyperglycemia, (2) low glucose tolerance, (3) insulin resistance, (4) obesity, (5) lipid disorders, (6) dyslipidemia, (7) hyperlipidemia, (8) hypertriglyceridemia, (9) hypercholesterolemia, (10) low HDL levels, (11) high LDL levels, (12) atherosclerosis and its sequelae, (13) vascular restenosis, (14) pancreatitis, (15) abdominal obesity, (16) neurodegenerative disease, (17) retinopathy, (18) nephropathy, (19) neuropathy, (20) Metabolic Syndrome, (21) hypertension and other conditions and disorders where insulin resistance is a component in a mammalian patient in need of such treatment is disclosed, comprising administering to the patient a compound in accordance with structural formula I in an amount that is effective to reduce the risk of developing said condition.
  • In another aspect of the invention, a method of treating a condition selected from the group consisting of (1) hyperglycemia, (2) low glucose tolerance, (3) insulin resistance, (4) obesity, (5) lipid disorders, (6) dyslipidemia, (7) hyperlipidemia, (8) hypertriglyceridemia, (9) hypercholesterolemia, (10) low HDL levels, (11) high LDL levels, (12) atherosclerosis and its sequelae, (13) vascular restenosis, (14) pancreatitis, (15) abdominal obesity, (16) neurodegenerative disease, (17) retinopathy, (18) nephropathy, (19) neuropathy, (20) Metabolic Syndrome, (21) hypertension and other conditions and disorders where insulin resistance is a component, in a mammalian patient in need of such treatment, comprising administering to the patient an effective amount of a compound as defined in structural formula I and a compound selected from the group consisting of:
  • (a) dipeptidyl peptidase-IV (DP-IV) inhibitors;
  • (b) insulin sensitizing agents selected from the group consisting of (i) PPARγ agonists, (ii) PPARα agonists, (iii) PPARα/γ dual agonists, and (iv) biguanides;
  • (c) insulin and insulin mimetics;
  • (d) sulfonylureas and other insulin secretagogues;
  • (e) α-glucosidase inhibitors;
  • (f) glucagon receptor antagonists;
  • (g) GLP-1, GLP-1 analogs, and GLP-1 receptor agonists;
  • (h) GIP, GIP mimetics, and GIP receptor agonists;
  • (i) PACAP, PACAP mimetics, and PACAP receptor 3 agonists;
  • (j) cholesterol lowering agents selected from the group consisting of
      • (i) HMG-CoA reductase inhibitors, (ii) sequestrants, (iii) nicotinyl alcohol, nicotinic acid and salts thereof, (iv) inhibitors of cholesterol absorption, (v) acyl CoA:cholesterol acyltransferase inhibitors, and (vi) anti-oxidants;
  • (k) PPARδ agonists;
  • (l) antiobesity compounds;
  • (m) ileal bile acid transporter inhibitors;
  • (n) anti-inflammatory agents, excluding glucocorticoids;
  • (O) protein tyrosine phosphatase 1B (PTP-1B) inhibitors; and
  • (p) antihypertensives including those acting on the angiotensin or renin systems, such as angiotensin converting enzyme inhibitors, angiotensin II receptor antagonists or renin inhibitors, such as captopril, cilazapril, enalapril, fosinopril, lisinopril, quinapril, ramapril, zofenopril, candesartan, cilexetil, eprosartan, irbesartan, losartan, tasosartan, telmisartan, and valsartan;
  • said compounds being administered to the patient in an amount that is effective to treat said condition.
  • Dipeptidyl peptidase-IV inhibitors that can be combined with compounds of structural formula I include those disclosed in WO 03/004498 (16 Jan. 2003); WO 03/004496 (16 Jan. 2003); EP 1 258 476 (20 Nov. 2002); WO 02/083128 (24 Oct. 2002); WO 02/062764 (15 Aug. 2002); WO 03/000250 (3 Jan. 2003); WO 03/002530 (9 Jan. 2003); WO 03/002531 (9
  • Jan. 2003); WO 03/002553 (9 Jan. 2003); WO 03/002593 (9 Jan. 2003); WO 03/000180 (3 Jan. 2003); and WO 03/000181 (3 Jan. 2003). Specific DP-IV inhibitor compounds include isoleucine thiazolidide; NVP-DPP728; P32/98; and LAF 237.
  • Antiobesity compounds that can be combined with compounds of structural formula I include fenfluramine, dexfenfluramine, phentermine, sibutramine, orlistat, neuropeptide Y1 or Y5 antagonists, cannabinoid CB1 receptor antagonists or inverse agonists, melanocortin receptor agonists, in particular, melanocortin-4 receptor agonists, ghrelin antagonists, and melanin-concentrating hormone (MCH) receptor antagonists. For a review of anti-obesity compounds that can be combined with compounds of structural formula I, see S. Chaki et al., “Recent advances in feeding suppressing agents: potential therapeutic strategy for the treatment of obesity,” Expert Opin. Ther. Patents, 11: 1677-1692 (2001)
  • Neuropeptide Y5 antagonists that can be combined with compounds of structural formula I include those disclosed in U.S. Pat. No. 6,335,345 (1 Jan. 2002) and WO 01/14376 (1 Mar. 2001); and specific compounds identified as GW 59884A; GW 569180A; LY366377; and CGP-71683A.
  • Cannabinoid CB1 receptor antagonists that can be combined with compounds of formula I include those disclosed in PCT Publication WO 03/007887; U.S. Pat. No. 5,624,941, such as rimonabant; PCT Publication WO 02/076949, such as SLV-319; U.S. Pat. No. 6,028,084; PCT Publication WO 98/41519; PCT Publication WO 00/10968; PCT Publication WO 99/02499; U.S. Pat. No. 5,532,237; and U.S. Pat. No. 5,292,736.
  • Melanocortin receptor agonists that can be combined with compounds of structural formula I include those disclosed in WO 03/009847 (6 Feb. 2003); WO 02/068388 (6 Sep. 2002); WO 99/64002 (16 Dec. 1999); WO 00/74679 (14 Dec. 2000); WO 01/70708 (27 Sep. 2001); and WO 01/70337 (27 Sep. 2001) as well as those disclosed in J. D. Speake et al., “Recent advances in the development of melanocortin-4 receptor agonists, Expert Opin. Ther. Patents, 12: 1631-1638 (2002).
  • In another aspect of the invention, a method of treating a condition selected from the group consisting of hypercholesterolemia, atherosclerosis, low HDL levels, high LDL levels, hyperlipidemia, hypertriglyceridemia, and dyslipidemia, in a mammalian patient in need of such treatment is disclosed, comprising administering to the patient a therapeutically effective amount of a compound as defined in structural formula I and an HMG-CoA reductase inhibitor.
  • More particularly, in another aspect of the invention, a method of treating a condition selected from the group consisting of hypercholesterolemia, atherosclerosis, low HDL levels, high LDL levels, hyperlipidemia, hypertriglyceridemia and dyslipidemia, in a mammalian patient in need of such treatment is disclosed, wherein the HMG-CoA reductase inhibitor is a statin.
  • Even more particularly, in another aspect of the invention, a method of treating a condition selected from the group consisting of hypercholesterolemia, atherosclerosis, low HDL levels, high LDL levels, hyperlipidemia, hypertriglyceridemia and dyslipidemia, in a mammalian patient in need of such treatment is disclosed, wherein the HMG-CoA reductase inhibitor is a statin selected from the group consisting of lovastatin, simvastatin, pravastatin, cerivastatin, fluvastatin, atorvastatin, itavastatin, and rosuvastatin.
  • In another aspect of the invention, a method of reducing the risk of developing a condition selected from the group consisting of hypercholesterolemia, atherosclerosis, low HDL levels, high LDL levels, hyperlipidemia, hypertriglyceridemia and dyslipidemia, and the sequelae of such conditions is disclosed comprising administering to a mammalian patient in need of such treatment a therapeutically effective amount of a compound as defined in structural formula I and an HMG-CoA reductase inhibitor.
  • In another aspect of the invention, a method for delaying the onset or reducing the risk of developing atherosclerosis in a human patient in need of such treatment is disclosed comprising administering to said patient an effective amount of a compound as defined in structural formula I and an HMG-CoA reductase inhibitor.
  • More particularly, a method for delaying the onset or reducing the risk of developing atherosclerosis in a human patient in need of such treatment is disclosed, wherein the HMG-CoA reductase inhibitor is a statin.
  • Even more particularly, a method for delaying the onset or reducing the risk of developing atherosclerosis in a human patient in need of such treatment is disclosed, wherein the HMG-Co A reductase inhibitor is a statin selected from the group consisting of: lovastatin, simvastatin, pravastatin, cerivastatin, fluvastatin, atorvastatin, itavastatin, and rosuvastatin.
  • Even more particularly, a method for delaying the onset or reducing the risk of developing atherosclerosis in a human patient in need of such treatment is disclosed, wherein the statin is simvastatin.
  • In another aspect of the invention, a method for delaying the onset or reducing the risk of developing atherosclerosis in a human patient in need of such treatment is disclosed, wherein the HMG-CoA reductase inhibitor is a statin and further comprising administering a cholesterol absorption inhibitor.
  • More particularly, in another aspect of the invention, a method for delaying the onset or reducing the risk of developing atherosclerosis in a human patient in need of such treatment is disclosed, wherein the HMG-Co A reductase inhibitor is a statin and the cholesterol absorption inhibitor is ezetimibe.
  • In another aspect of the invention, a pharmaceutical composition is disclosed which comprises
  • (1) a compound according to structural formula I,
    (2) a compound selected from the group consisting of:
  • (a) DP-IV inhibitors;
  • (b) insulin sensitizing agents selected from the group consisting of (i) PPARγ agonists; (ii) PPARα agonists, (iii) PPARα/γ dual agonists, and (iv) biguanides;
  • (c) insulin and insulin mimetics;
  • (d) sulfonylureas and other insulin secretagogues;
  • (e) α-glucosidase inhibitors;
  • (f) glucagon receptor antagonists;
  • (g) GLP-1, GLP-1 analogs, and GLP-1 receptor agonists;
  • (h) GIP, GIP mimetics, and GIP receptor agonists;
  • (i) PACAP, PACAP mimetics, and PACAP receptor 3 agonists;
  • k) cholesterol lowering agents selected from the group consisting of (i) HMG-CoA reductase inhibitors, (ii) sequestrants, (iii) nicotinyl alcohol, nicotinic acid or a salt thereof, (iv) inhibitors of cholesterol absorption, (v) acyl CoA:cholesterol acyltransferase inhibitors, and (vi) anti-oxidants;
  • (k) PPARδ agonists;
  • (l) antiobesity compounds;
  • (m) ileal bile acid transporter inhibitors;
  • (n) anti-inflammatory agents other than glucocorticoids;
  • (O) protein tyrosine phosphatase 1B (PTP-1B) inhibitors; and
  • (p) antihypertensives including those acting on the angiotensin or renin systems, such as angiotensin converting enzyme inhibitors, angiotensin II receptor antagonists or renin inhibitors, such as captopril, cilazapril, enalapril, fosinopril, lisinopril, quinapril, ramapril, zofenopril, candesartan, cilexetil, eprosartan, irbesartan, losartan, tasosartan, telmisartan, and valsartan; and
  • (3) a pharmaceutically acceptable carrier.
  • The compounds of the present invention may be administered in the form of a pharmaceutically acceptable salt. The term “pharmaceutically acceptable salt” refers to salts prepared from pharmaceutically acceptable non-toxic bases or acids including inorganic or organic bases and inorganic or organic acids. Salts of basic compounds encompassed within the term “pharmaceutically acceptable salt” refer to non-toxic salts of the compounds of this invention which are generally prepared by reacting the free base with a suitable organic or inorganic acid. Representative salts of basic compounds of the present invention include, but are not limited to, the following: acetate, benzenesulfonate, benzoate, bicarbonate, bisulfate, bitartrate, borate, bromide, camsylate, carbonate, chloride, clavulanate, citrate, dihydrochloride, edetate, edisylate, estolate, esylate, fumarate, gluceptate, gluconate, glutamate, glycollylarsanilate, hexylresorcinate, hydrabamine, hydrobromide, hydrochloride, hydroxynaphthoate, iodide, isothionate, lactate, lactobionate, laurate, malate, maleate, mandelate, mesylate, methylbromide, methylnitrate, methylsulfate, mucate, napsylate, nitrate, N-methylglucamine ammonium salt, oleate, oxalate, pamoate (embonate), palmitate, pantothenate, phosphate/diphosphate, polygalacturonate, salicylate, stearate, sulfate, subacetate, succinate, tannate, tartrate, teoclate, tosylate, triethiodide and valerate. Furthermore, where the compounds of the invention carry an acidic moiety, suitable pharmaceutically acceptable salts thereof include, but are not limited to, salts derived from inorganic bases including aluminum, ammonium, calcium, copper, ferric, ferrous, lithium, magnesium, manganic, mangamous, potassium, sodium, zinc, and the like. Particularly preferred are the ammonium, calcium, magnesium, potassium, and sodium salts. Salts derived from pharmaceutically acceptable organic non-toxic bases include salts of primary, secondary, and tertiary amines, cyclic amines, and basic ion-exchange resins, such as arginine, betaine, caffeine, choline, N,N-dibenzylethylenediamine, diethylamine, 2-diethylaminoethanol, 2-dimethylaminoethanol, ethanolamine, ethylenediamine, N-ethylmorpholine, N-ethylpiperidine, glucamine, glucosamine, histidine, hydrabamine, isopropylamine, lysine, methylglucamine, morpholine, piperazine, piperidine, polyamine resins, procaine, purines, theobromine, triethylamine, trimethylamine, tripropylamine, tromethamine, and the like.
  • Also, in the case of a carboxylic acid (—COOH) or alcohol group being present in the compounds of the present invention, pharmaceutically acceptable esters of carboxylic acid derivatives, such as methyl, ethyl, or pivaloyloxymethyl, or acyl derivatives of alcohols, such as acetate or maleate, can be employed. Included are those esters and acyl groups known in the art for modifying the solubility or hydrolysis characteristics for use as sustained-release or prodrug formulations.
  • It will be understood that, as used herein, references to the compounds of structural formula I are meant to also include the pharmaceutically acceptable salts, and also salts that are not pharmaceutically acceptable when they are used as precursors to the free compounds or their pharmaceutically acceptable salts or in other synthetic manipulations.
  • Solvates, and in particular, the hydrates of the compounds of structural formula I are included in the present invention as well.
  • The compounds described herein are selective inhibitors of the 11β-HSD1 enzyme. Thus, the present invention relates to the use of the 11β-HSD1 inhibitors for inhibiting the reductase activity of 11β-hydroxysteroid dehydrogenase, which is responsible for the conversion of cortisone to cortisol. Excess cortisol is associated with numerous disorders, including NIDDM, obesity, dyslipidemia, insulin resistance and hypertension. Administration of the compounds of the present invention decreases the level of cortisol and other 11β-hydroxysteroids in target tissues, thereby reducing the effects of excessive amounts of cortisol and other 11β-hydroxysteroids. Inhibition of 11β-HSD1 can be used to treat and control diseases mediated by abnormally high levels of cortisol and other 11β-hydroxysteroids, such as NIDDM, obesity, hypertension and dyslipidemia. Inhibition of 11β-HSD1 activity in the brain such as to lower cortisol levels may also be useful to treat or reduce anxiety, depression, and cognitive impairment.
  • The present invention includes the use of an 11β-HSD1 inhibitor for the treatment, control, amelioration, prevention, delaying the onset of or reducing the risk of developing the diseases and conditions that are described herein, as mediated by excess or uncontrolled amounts of cortisol and/or other corticosteroids in a mammalian patient, particularly a human, by the administration of an effective amount of a compound of structural formula I or a pharmaceutically acceptable salt or solvate thereof. Inhibition of the 11β-HSD1 enzyme limits the conversion of cortisone, which is normally inert, to cortisol, which can cause or contribute to the symptoms of these diseases and conditions if present in excessive amounts.
    • NIDDM and Hypertension:
  • The compounds of this invention are selective inhibitors of 11β-HSD1 over 11β-HSD2. While the inhibition of 11β-HSD1 is useful for reducing cortisol levels and treating conditions related thereto, inhibition of 11β-HSD2 is associated with serious side effects, such as hypertension.
  • Cortisol is an important and well recognized anti-inflammatory hormone, which also acts as an antagonist to the action of insulin in the liver, such that insulin sensitivity is reduced, resulting in increased gluconeogenesis and elevated levels of glucose in the liver. Patients who already have impaired glucose tolerance have a greater probability of developing Type 2 diabetes in the presence of abnormally high levels of cortisol.
  • High levels of cortisol in tissues where the mineralocorticoid receptor is present often lead to hypertension. Inhibition of 11β-HSD1 shifts the ratio of cortisol and cortisone in specific tissues in favor of cortisone.
  • Administration of a therapeutically effective amount of an 11β-HSD1 inhibitor is effective in treating, controlling and ameliorating the symptoms of NIDDM, and administration of a therapeutically effective amount of an 11β-HSD1 inhibitor on a regular basis delays or prevents the onset of NIDDM, particularly in humans.
    • Cushing's Syndrome:
  • The effect of elevated levels of cortisol is also observed in patients who have Cushing's Syndrome, which is a metabolic disease characterized by high levels of cortisol in the blood stream. Patients with Cushing's Syndrome often develop NIDDM.
    • Obesity Metabolic Syndrome Dyslipidemia:
  • Excessive levels of cortisol have been associated with obesity, perhaps due to increased hepatic gluconeogenesis. Abdominal obesity is closely associated with glucose intolerance, hyperinsulinemia, hypertriglyceridemia, and other factors of Metabolic Syndrome, such as high blood pressure, elevated VLDL and reduced HDL. Montague et al., Diabetes, 2000, 49: 883-888. Thus, the administration of an effective amount of an 11β-HSD1 inhibitor is useful in the treatment or control of obesity. Long-term treatment with an 11β-HSD1 inhibitor is also useful in delaying or preventing the onset of obesity, especially if the patient uses an 11β-HSD1 inhibitor in combination with controlled diet and exercise.
  • By reducing insulin resistance and maintaining serum glucose at normal concentrations, compounds of the present invention also have utility in the treatment and prevention of conditions that accompany Type II diabetes and insulin resistance, including the Metabolic Syndrome or Syndrome X, obesity, reactive hypoglycemia and diabetic dyslipidemia.
    • Cognition and Dementia:
  • Excessive levels of cortisol in the brain may also result in neuronal loss or dysfunction through the potentiation of neurotoxins. Cognitive impairment has been associated with aging, and excess levels of cortisol in the brain. See J. R. Seckl and B. R. Walker, Endocrinology, 2001, 142: 1371-1376, and references cited therein. Administration of an effective amount of an 11β-HSD1 inhibitor results in the reduction, amelioration, control or prevention of cognitive impairment associated with aging and of neuronal dysfunction. Inhibitors of 11β-HSD1 may also be useful to treat anxiety and depression.
    • Atherosclerosis:
  • As described above, inhibition of 113-HSD1 activity and a reduction in the amount of cortisol are beneficial in treating or controlling hypertension. Since hypertension and dyslipidemia contribute to the development of atherosclerosis, administration of a therapeutically effective amount of an 11β-HSD1 inhibitor of the present invention may be especially beneficial in treating, controlling, delaying the onset of or preventing atherosclerosis.
    • Effects on Pancreas:
  • Inhibition of 11β-HSD1 activity in isolated murine pancreatic 1-cells improves glucose stimulated insulin secretion (B. Davani et al., J. Biol. Chem., 2000, 275: 34841-34844). Glucocorticoids have been shown to reduce insulin secretion in vivo. (B. Billaudel et al., Horm. Metab. Res., 1979, 11: 555-560).
    • Reduction of Intraocular Pressure:
  • Recent data suggests a connection between the levels of glucocorticoid target receptors and the 11β-HSD enzymes and the susceptibility to glaucoma (J. Stokes et al., Invest. Ophthamol., 2000, 41: 1629-1638). Therefore, inhibition of 11β-HSD1 activity is useful in reducing intraocular pressure in the treatment of glaucoma.
    • Immunomodulation:
  • In certain disease states, such as tuberculosis, psoriasis, and even under conditions of excessive stress, high glucocorticoid activity shifts the immune response to a humoral response, when in fact a cell based response may be more beneficial to the patient. Inhibition of 11β-HSD1 activity and the attendant reduction in glucocorticoid levels shifts the immune response toward a cell based response. See D. Mason, Immunology Today, 1991, 12: 57-60, and G. A. W. Rook, Bailliér's Clin. Endocrinol. Metab., 1999, 13: 576-581.
    • Osteoporosis:
  • Glucocorticoids can inhibit bone formation, which can result in a net bone loss. 11β-HSD1 has a role in bone resorption. Inhibition of 11β-HSD1 is beneficial in preventing bone loss due to osteoporosis. See C. H. Kim et al., J. Endocrinol., 1999, 162: 371-379; C. G. Bellows et al., Bone, 1998, 23: 119-125; and M. S. Cooper et al., Bone, 2000, 27: 375-381.
    • Other Utilities:
  • The following diseases, disorders and conditions can be treated, controlled, prevented or delayed, by treatment with the compounds of this invention: (1) hyperglycemia, (2) low glucose tolerance, (3) insulin resistance, (4) obesity, (5) lipid disorders, (6) dyslipidemia, (7) hyperlipidemia, (8) hypertriglyceridemia, (9) hypercholesterolemia, (10) low HDL levels, (11) high LDL levels, (12) atherosclerosis and its sequelae, (13) vascular restenosis, (14) pancreatitis, (15) abdominal obesity, (16) neurodegenerative disease, (17) retinopathy, (18) nephropathy, (19) neuropathy, (20) Metabolic Syndrome, (21) hypertension and other disorders where insulin resistance is a component.
  • The above diseases and conditions can be treated using the compounds of structural formula I, or the compound can be administered to prevent or reduce the risk of developing the diseases and conditions described herein. Since concurrent inhibition of 11β-HSD2 may have deleterious side effects or may actually increase the amount of cortisol in the target tissue where reduction of cortisol is desired, selective inhibitors of 11β-HSD1 with little or no inhibition of 11β-HSD2 are desirable.
  • The 11β-HSD1 inhibitors of structural formula I generally have an inhibition constant IC50 of less than about 500 nM, and preferably less than about 100 nM. Generally, the IC50 ratio for 11β-HSD2 to 11β-HSD1 of a compound is at least about two or more, and preferably about ten or greater. Even more preferred are compounds with an IC50 ratio for 11β-HSD2 to 11β-HSD1 of about 100 or greater. For example, compounds of the present invention ideally demonstrate an inhibition constant IC50 against 11β-HSD2 greater than about 1000 nM, and preferably greater than 5000 nM.
  • Compounds of structural formula I may be used in combination with one or more other drugs in the treatment, prevention, suppression or amelioration of diseases or conditions for which compounds of structural formula I or the other drugs have utility. Typically the combination of the drugs is safer or more effective than either drug alone, or the combination is safer or more effective than would be expected based on the additive properties of the individual drugs. Such other drug(s) may be administered, by a route and in an amount commonly used contemporaneously or sequentially with a compound of structural formula I. When a compound of structural formula I is used contemporaneously with one or more other drugs, a combination product containing such other drug(s) and the compound of structural formula I is preferred. However, combination therapy also includes therapies in which the compound of structural formula I and one or more other drugs are administered on different overlapping schedules. It is contemplated that when used in combination with other active ingredients, the compound of the present invention or the other active ingredient or both may be used effectively in lower doses than when each is used alone. Accordingly, the pharmaceutical compositions of the present invention include those that contain one or more other active ingredients, in addition to a compound of structural formula I.
  • Examples of other active ingredients that may be administered in combination with a compound of structural formula I, and either administered separately or in the same pharmaceutical composition, include, but are not limited to:
  • (a) dipeptidyl peptidase IV (DP-IV) inhibitors;
  • (b) insulin sensitizing agents including (i) PPARγ agonists such as the glitazones (e.g. troglitazone, pioglitazone, englitazone, MCC-555, rosiglitazone, and the like) and other PPAR ligands, including PPARα/γ dual agonists, such as KRP-297, and PPARα agonists such as gemfibrozil, clofibrate, fenofibrate and bezafibrate, and (ii) biguanides, such as metformin and phenformin;
  • (c) insulin or insulin mimetics;
  • (d) sulfonylureas and other insulin secretagogues such as tolbutamide, glipizide, meglitinide and related materials;
  • (e) α-glucosidase inhibitors, such as acarbose;
  • (f) glucagon receptor antagonists such as those disclosed in WO 98/04528, WO 99/01423, WO 00/39088 and WO 00/69810;
  • (g) GLP-1, GLP-1 analogs, and GLP-1 receptor agonists such as those disclosed in WO00/42026 and WO00/59887;
  • (h) GIP, GIP mimetics such as those disclosed in WO00/58360, and GIP receptor agonists;
  • (i) PACAP, PACAP mimetics, and PACAP receptor 3 agonists such as those disclosed in WO 01/23420;
  • k) cholesterol lowering agents such as (i) HMG-CoA reductase inhibitors (lovastatin, simvastatin, pravastatin, cerivastatin, fluvastatin, atorvastatin, itavastatin, rosuvastatin, and other statins), (ii) bile-acid sequestrants (cholestyramine, colestipol, and dialkylaminoalkyl derivatives of a cross-linked dextran), (iii) nicotinyl alcohol, nicotinic acid or a salt thereof, (iv) inhibitors of cholesterol absorption, such as ezetimibe and beta-sitosterol, (v) acyl CoA:cholesterol acyltransferase inhibitors, such as, for example, avasimibe, and (vi) anti-oxidants, such as probucol;
  • (k) PPARδ agonists, such as those disclosed in WO97/28149;
  • (l) antiobesity compounds such as fenfluramine, dexfenfluramine, phentermine, sibutramine, orlistat, neuropeptide Y1 or Y5 antagonists, CB1 receptor inverse agonists and antagonists, β3 adrenergic receptor agonists, melanocortin-receptor agonists, in particular melanocortin-4 receptor agonists, ghrelin antagonists, and melanin-concentrating hormone (MCH) receptor antagonists;
  • (m) ileal bile acid transporter inhibitors;
  • (n) agents intended for use in inflammatory conditions other than glucocorticoids, such as aspirin, non-steroidal anti-inflammatory drugs, azulfidine, and selective cyclooxygenase-2 inhibitors;
  • (O) protein tyrosine phosphatase 1B (PTP-1B) inhibitors; and
  • (p) antihypertensives including those acting on the angiotensin or renin systems, such as angiotensin converting enzyme inhibitors, angiotensin II receptor antagonists or renin inhibitors, such as captopril, cilazapril, enalapril, fosinopril, lisinopril, quinapril, ramapril, zofenopril, candesartan, cilexetil, eprosartan, irbesartan, losartan, tasosartan, telmisartan, and valsartan.
  • The above combinations include a compound of structural formula I, or a pharmaceutically acceptable salt or solvate thereof, with one or more other active compounds. Non-limiting examples include combinations of compounds of structural formula I with two or more active compounds selected from biguanides, sulfonylureas, HMG-CoA reductase inhibitors, PPAR agonists, PTP-1B inhibitors, DP-IV inhibitors, and anti-obesity compounds.
  • Any suitable route of administration may be employed for providing a mammal, especially a human, with an effective dose of a compound of the present invention. For example, oral, rectal, topical, parenteral, ocular, pulmonary, nasal and the like may be employed. Dosage forms include tablets, troches, dispersions, suspensions, solutions, capsules, creams, ointments, aerosols and the like. Preferably the compound of structural formula I is administered orally.
  • The effective dosage of the active ingredient varies depending on the particular compound employed, the mode of administration, the condition being treated and the severity of the condition. Such dosages may be ascertained readily by a person skilled in the art.
  • When treating or preventing the diseases and conditions described herein, for which compounds of structural formula I are indicated, satisfactory results are obtained when the compounds of the invention are administered at a daily dosage of from about 0.1 to about 100 milligram per kilogram (mpk) of body weight, preferably given as a single daily dose or in divided doses about two to six times a day. The total daily dosage thus ranges from about 0.1 mg to about 1000 mg, preferably from about 1 mg to about 50 mg. In the case of a typical 70 kg adult human, the total daily dose will range from about 7 mg to about 350 mg. This dosage may be adjusted to provide the optimal therapeutic response.
  • Another aspect of the present invention relates to a pharmaceutical composition which comprises a compound of structural formula I, or a pharmaceutically acceptable salt or solvate thereof, in combination with a pharmaceutically acceptable carrier.
  • The compositions include compositions suitable for oral, rectal, topical, parenteral (including subcutaneous, intramuscular, and intravenous), ocular (ophthalmic), transdermal, pulmonary (nasal or buccal inhalation), or nasal administration, although the most suitable route in any given case will depend on the nature and severity of the condition being treated and the active ingredient. They may be conveniently presented in unit dosage form and prepared by any of the methods well-known in the art of pharmacy.
  • The compound of structural formula I can be combined with the pharmaceutical carrier according to conventional pharmaceutical compounding techniques. Carriers take a wide variety of forms. For example, carriers for oral liquid compositions include, e.g., water, glycols, oils, alcohols, flavoring agents, preservatives, coloring agents and other components used in the manufacture of oral liquid suspensions, elixirs and solutions. Carriers such as starches, sugars and microcrystalline cellulose, diluents, granulating agents, lubricants, binders, disintegrating agents and the like are used to prepare oral solid dosage forms, e.g., powders, hard and soft capsules and tablets. Solid oral preparations are preferred over oral liquids.
  • The oral solid dosage forms may also contain a binder such as gum tragacanth, acacia, corn starch or gelatin; excipients such as dicalcium phosphate; a disintegrating agent such as corn starch, potato starch, alginic acid; a lubricant such as magnesium stearate; and a sweetening agent such as sucrose, lactose or saccharin. Capsules may also contain a liquid carrier such as a fatty oil.
  • Various other materials may be present to act as coatings or to modify the physical form of the dosage unit. For instance, tablets may be coated with shellac, sugar or both.
  • Tablets may be coated by standard aqueous or nonaqueous techniques. The typical percentage of active compound in these compositions may, of course, be varied from about 2 percent to about 60 percent on a w/w basis. Thus, tablets contain a compound of structural formula I or a salt or hydrate thereof in an amount ranging from as low as about 0.1 mg to as high as about 1.5 g, preferably from as low as about 1.0 mg to as high as about 500 mg, and more preferably from as low as about 10 mg to as high as about 100 mg.
  • Oral liquids such as syrups or elixirs may contain, in addition to the active ingredient, sucrose as a sweetening agent, methyl and propylparabens as preservatives, a dye and a flavoring such as cherry or orange flavor.
  • Parenterals are typically in the form of a solution or suspension, typically prepared with water, and optionally including a surfactant such as hydroxypropylcellulose. Dispersions can be prepared in glycerol, liquid polyethylene glycols and mixtures thereof in oils. Typically preparations that are in diluted form also contain a preservative.
  • The pharmaceutical injectable dosage forms, including aqueous solutions and dispersions and powders for the extemporaneous preparation of injectable solutions or dispersions, are also sterile and must be fluid to the extent that easy syringability exists; they must be stable under the conditions of manufacture and storage and are usually preserved. The carrier thus includes the solvent or dispersion medium containing, for example, water, ethanol, polyol (e.g. glycerol, propylene glycol and liquid polyethylene glycol), suitable mixtures thereof, and vegetable oils.
    • Assays: Measurement of Inhibition Constants:
  • In vitro enzymatic activity was assessed for test compounds via a Scintillation Proximity Assay (SPA). In short, tritiated-cortisone substrate, NADPH cofactor and titrated compound of structural formula I were incubated with 11β-HSD1 enzyme at 37° C. to allow conversion to cortisol to progress. Following this incubation, a preparation of protein A coated SPA beads, pre-blended with anti-cortisol monoclonal antibody and a non-specific 11β-HSD inhibitor, such as 18β-glycyrrhetinic acid, was added to each well. The mixture was shaken at 15° C. and was then read on a liquid scintillation counter suitable for 96 well plates. Percent inhibition was calculated relative to a non-inhibited control well and IC50 curves were generated. This assay was similarly applied to 11β-HSD2, whereby tritiated cortisol and NAD were used as the substrate and cofactor, respectively. To begin the assay, 40 μL of substrate (25 nM 3H-Cortisone+1.25 mM NADPH in 50 mM HEPES Buffer, pH 7.4) was added to designated wells on a 96-well plate. The compound was dissolved in DMSO at 10 mM followed by a subsequent 50 fold dilution in DMSO. The diluted material was then titrated 4 fold, seven times. 1 μL of each titrated compound was then added in duplicate to the substrate. To start the reaction, 10 μL of 11β-HSD1 microsome from CHO transfectants was added to each well at the appropriate concentration to yield approximately 10% conversion of the starting material. For ultimate calculation of percent inhibition, a series of wells were added that represented the assay minimum and maximum: one set that contained substrate without compound or enzyme (background), and another set that contained substrate and enzyme without any compound (maximum signal). The plates were spun briefly at a low speed in a centrifuge to pool the reagents, sealed with an adhesive strip, mixed gently, and incubated at 37° C. for 2 h. After incubation, 45 μL of SPA beads, pre-suspended with anti-cortisol monoclonal antibody and a compound of formula I, were added to each well. The plates were resealed and shaken gently for greater than 1.5 h at 15° C. Data were collected on a plate based liquid scintillation counter such as a Topcount. To control for inhibition of anti-cortisol antibody/cortisol binding, substrate spiked with 1.25 nM [3]H cortisol was added to designated single wells. 1 μL of 200 μM compound was added to each of these wells, along with 10 μL of buffer instead of enzyme. Any calculated inhibition was due to compound interfering with the cortisol binding to the antibody on the SPA beads.
    • Assays: Measurement of In Vivo Inhibition:
  • In general terms, the test compound was dosed orally to a mammal and a prescribed time interval was allowed to elapse, usually between 1 and 24 h. Tritiated cortisone was injected intravenously, followed several min later by blood collection. Steroids were extracted from the separated serum and analyzed by HPLC. The relative levels of 3H-cortisone and its reduction product, 3H-cortisol, were determined for the compound and vehicle-dosed control groups. The absolute conversion, as well as the percentage of inhibition, was calculated from these values.
  • More specifically, compounds were prepared for oral dosing by dissolving them in vehicle (5% hydroxypropyl-beta-cyclodextrin v/v H2O, or equivalent) at the desired concentration to allow dosing at typically 10 mg per kg. Following an overnight fasting, the solutions were dosed to ICR mice (obtained from Charles River) by oral gavage, 0.5 mL per dose per animal, with three animals per test group.
  • After the desired time had passed, routinely either 4 or 16 h, 0.2 mL of 3 μM 3H-cortisone in dPBS was injected by tail vein. The animal was caged for two min followed by euthanasia in a CO2 chamber. Upon expiration, the mouse was removed and blood was collected by cardiac puncture. The blood was set aside in a serum separation tube for no less than 30 min at room temperature to allow for adequate coagulation. After the incubation period, blood was separated into serum by centrifugation at 3000×g, 4° C., for 10 min.
  • To analyze the steroids in the serum, they were first extracted with organic solvent. A 0.2 mL volume of serum was transferred to a clean microcentrifuge tube. To this a 1.0 mL volume of ethyl acetate was added, followed by vigorous vortexing for 1 min. A quick spin on a microcentrifuge pelleted the aqueous serum proteins and clarified the organic supernatant. 0.85 mL of the upper organic phase was transferred to a fresh microcentrifuge tube and dried. The dried sample was resuspended in 0.250 mL of DMSO containing a high concentration of cortisone and cortisol for analysis by HPLC.
  • A 0.200 mL sample was injected onto a Metachem Inertsil C-18 chromatography column equilibrated in 30% methanol. A slow linear gradient to 50% methanol separated the target steroids; simultaneous monitoring by UV at 254 nm of the cold standards in the resuspension solution acted as an internal standard. The tritium signal was collected by a radiochromatography detector that uploaded data to software for analysis. The percent conversion of 3H-cortisone to 3H-cortisol was calculated as the ratio of AUC for cortisol over the combined AUC for cortisone and cortisol.
    • Preparation of Compounds of the Invention:
  • The compounds of structural formula I of the present invention can be prepared according to the procedures of the following Schemes and Examples, using appropriate materials and are further exemplified by the following specific examples. The compounds illustrated in the examples are not, however, to be construed as forming the only genus that is considered as the invention. The Examples further illustrate details for the preparation of the compounds of the present invention. Those skilled in the art will readily understand that known variations of the conditions and processes of the following preparative procedures can be used to prepare these compounds. The instant compounds are generally isolated in the their neutral form, but the triazole moeity can be further converted into a pharmaceutically acceptable salt by dissolution in an organic solvent followed by addition of the appropriate acid and subsequent evaporation, precipitation, or crystallization. All temperatures are degrees Celsius unless otherwise noted. Mass spectra (MS) were measured by electrospray ion-mass spectroscopy (ESMS).
  • The phrase “standard peptide coupling reaction conditions” means coupling a carboxylic acid with an amine using an acid activating agent such as EDC, DCC, and BOP in an inert solvent such as dichloromethane in the presence of a catalyst such as HOBT. The use of protecting groups for the amine and carboxylic acid functionalities to facilitate the desired reaction and minimize undesired reactions is well documented. Conditions required to remove protecting groups are found in standard textbooks such as Greene, T, and Wuts, P. G. M., Protective Groups in Organic Synthesis, John Wiley & Sons, Inc., New York, N.Y., 1991. Cbz and BOC are commonly used protecting groups in organic synthesis, and their removal conditions are known to those skilled in the art.
    • Abbreviations Used in the Description of the Preparation of the Compounds of the Present Invention:
  • AIBN 2,2′-azobisisobutyronitrile
    BOC t-butyloxycarbonyl
    BBr3 boron tribromide
    9-BBN 9-borabicyclo[3.3.1]nonane
    Bn benzyl
    nBuLi n-butyl lithium
    Cbz benzyloxycarbonyl
    CDI 1,1′-carbonyldiimidazole
    MeOTf methyl trifluoromethanesulfonate
    CH2Cl2 dichloromethane
    CH2I2 diiodomethane
    (COCl)2 oxalyl chloride
    Cs2CO3 cesium carbonate
    DAST (diethylamino)sulfur trifluoride
    DMAP 4-(dimethylamino)pyridine
    DMF N,N-dimethylformamide
    Et ethyl
    Et3N triethylamine
    EtOAc ethyl acetate
    Et2Zn diethylzinc
    H2O2 hydrogen peroxide
    Me methyl
    MeCN acetonitrile
    MeOH methanol
    mCPBA meta-chloroperbenzoic acid
    MS mass spectrum
    NaBH4 sodium borohydride
    NaHCO3 sodium hydrogencarbonate
    NaOAc sodium acetate
    NBS N-bromosuccinimide
    Ph phenyl
    PyBROP bromotripyrrolidinophosphonium
    hexafluorophosphate
    PPh3 triphenylphosphine
    Pyr pyridine
    SOCl2 thionyl chloride
    TFA trifluoroacetic acid
    TFFH N,N,N′,N′-tetramethylformamidinium
    hexafluorophosphate
    THF tetrahydrofuran
    TLC thin-layer chromatography
    TsOH p-toluenesulfonic acid
  • Reaction Schemes 1-5 illustrate the methods employed in the synthesis of the compounds of the present invention of structural formula I. All substituents are as defined above unless indicated otherwise.
  • Reaction Scheme 1 illustrates a key step in the synthesis of the novel compounds of structural formula I of the present invention. As shown in reaction Scheme 1, a secondary amide (1-1) (N-Me or N-Et preferred) can be methylated by heating with neat methyl triflate in order to provide an iminoether (1-2). Alternatively other methylating reagents such as methyl iodide or methyl sulfate may be used neat or in a non-nucleophilic organic solvent. As shown in Scheme 1, a bicyclo[2.2.2]octane-1-carboxylic acid (1-3) is converted to an acyl hydrazide (1-4) by using the coupling reagent TFFH and hydrazine in the presence of a tertiary amine base such as triethylamine. Alternatively, other coupling reagents commonly used for preparing amides may be used for this transformation along with hydrazine. Alternatively, a bicyclo[2.2.2]octane-1-carboxylic ester can be heated with hydrazine to prepare acyl hydrazides (1-4). The acyl hydrazide (1-4) and iminoether (1-2) thus produced can be heated together in an inert high boiling organic solvent such as toluene in the presence of a tertiary amine base such as triethylamine to provide bicyclo[2.2.2]octyltriazoles (1-5) of structural formula I.
  • Figure US20090181994A1-20090716-C00007
  • Alternatively, the reaction can be conducted in the inverse manner as described by reaction Scheme 2. In this procedure a secondary amide (2-1) is prepared from a bicyclo[2.2.2]octane-1-carboxylic acid using a standard peptide coupling reaction. This compound is methylated to form the iminoether (2-2) and reacted with an acyl hydrazide as described for reaction Scheme 1 to provide bicyclo[2.2.2]octyltriazoles (2-3) of structural formula I.
  • Figure US20090181994A1-20090716-C00008
  • Reaction Scheme 3 describes an alternate approach to compounds of the present invention of structural formula I, in which the key step is the palladium catalyzed Suzuki coupling reaction between a bicyclo[2.2.2]octylbromotriazole (3-1) and an aryl boronic acid to produce triazoles (3-2) of structural formula I. The preferred conditions use tetrakis(triphenylphosphine)palladium(0) as the catalyst in DMF solvent with cesium carbonate, but other catalysts and conditions may be employed, as recognized by those skilled in the art.
  • Figure US20090181994A1-20090716-C00009
  • Reaction Scheme 4 describes yet another synthetic approach to the formation of compounds of structural formula I. Using this procedure, 4-(bicyclo[2.2.2]octyl)oxadiazoles (4-1) are dehydratively condensed with methylamine, either neat in a melt with methylammonium trifluoroacetate or in buffered MeOH solution. These reactions are best performed at high temperatures in a high pressure reactor to prevent the loss of methylamine.
  • Figure US20090181994A1-20090716-C00010
  • Reaction Scheme 5 describes yet another synthetic approach to the formation of compounds of structural formula I. Using this procedure, bicyclo[2.2.2]octylcarboxamides (5-1) are converted to iminochlorides (5-2), using a reagent such as oxalyl chloride, thionyl chloride, phosphorus oxychloride or phosphorus pentachloride, optionally in the presence of DMF. The iminochloride (5-2) is condensed with an aryl tetrazole in a high boiling inert organic solvent such as toluene to provide the triazole (5-3).
  • Figure US20090181994A1-20090716-C00011
    • Preparation of [2.2.2]Bicyclooctyl Intermediates:
  • The procedures used in the preparation of [2.2.2]bicyclooctyl intermediates for use in the preparation of compounds of the present invention are provided below.
  • Intermediate Schemes 1-4 describe the preparation of oxadiazoles, which are important intermediates for the synthesis of compounds of structural formula I. They can be converted into compounds of structural formula I using, for example, the reactions described in reaction Scheme 4.
  • Intermediate Scheme 1 shows a preferred method for the preparation of oxadiazoles via the dehydration of diacyl hydrazides using a dehydrating reagent such as thionyl chloride. Alternatively, other dehydrating reagents such as phosphorus oxychloride, phosphorus pentachloride or oxalyl chloride may be employed. The diacyl hydrazides may be prepared preferentially from a hydrazide and an activated acid, such as an acid chloride, in the presence of a tertiary amine base. Alternatively, standard peptide coupling reactions may be employed to prepare the diacyl hydrazide from a hydrazide and a carboxylic acid.
  • Intermediate Scheme 2 shows a useful reagent for the dehydration of diacyl hydrazides to oxadiazoles, namely, 2-chloro-1,3-dimethyl-4,5-dihydro-1H-imidazol-3-ium chloride. This reagent in a non-polar solvent (methylene chloride is preferred) along with a tertiary amine base (triethylamine is preferred) gives the desired oxadiazole intermediates in an efficient manner.
  • Intermediate Scheme 3 shows a preferred reagent for the one pot formation (from a hydrazide and a carboxylic acid) and dehydration of diacyl hydrazides to oxadiazoles: 2-chloro-1,3-dimethyl-4,5-dihydro-1H-imidazol-3-ium chloride. This reagent in a non-polar solvent (methylene chloride is preferred) along with a tertiary amine base (triethylamine is preferred) gives the desired oxadiazole intermediates in an efficient manner.
  • Intermediate Scheme 4 shows an efficient method for the formation of oxadiazoles from secondary amides and hydrazides. The secondary amide (N-Me or N-Et preferred) can be methylated by heating with neat methyl triflate in order to provide an iminoether. Alternatively other methylating reagents such as methyl iodide or methyl sulfate may be used neat or in a non-nucleophilic organic solvent. Heating the iminoether thus formed in a high boiling inert organic solvent in the presence of a hydrazide affords oxadiazoles as shown in the Scheme.
  • Figure US20090181994A1-20090716-C00012
  • Figure US20090181994A1-20090716-C00013
  • Figure US20090181994A1-20090716-C00014
  • Figure US20090181994A1-20090716-C00015
  • Intermediate Scheme 5 shows a preferred method for the synthesis of bicyclo[2.2.2]octane-1-carboxylic acid.
  • Figure US20090181994A1-20090716-C00016
  • Intermediate Schemes 6 and 7 show preferred methods for the preparation of bicyclo[2.2.2]octane-1-carboxylic acids with a heteroaryl group at the R3 position as given by structural formula I. Oxadiazoles at the R3 position may be prepared by the condensation of a bicyclo[2.2.2]octyl-1-carboxylic acid with an amidoxime as shown in Intermediate Scheme 6. A useful reagent for this coupling is CDI. Alternatively, other reagents useful for dehydration or peptide coupling reactions may be employed. Intermediate Scheme 7 illustrates a preferred method for the synthesis of an intermediate of compounds of structural formula I bearing a thiazole group at the R3 position.
  • Figure US20090181994A1-20090716-C00017
  • Figure US20090181994A1-20090716-C00018
  • Intermediate Schemes 8-14 show preferred methods for the preparation of bicyclo[2.2.2]octane-1-carboxylic acids intermediates in the synthesis of compounds of structural formula I with various alkyl or alkenyl or substituted alkyl groups at the R3 position. A key reaction is the Wittig reaction performed on a bicyclo[2.2.2]octane-1-carboxaldehyde, as shown in Intermediate Scheme 8. The double bond in the product of this reaction may be hydrogenated to generate an alkyl group of varying length and character (which will become the R3 substituent in structural formula I), depending on the Wittig reagent, as shown in Intermediate Scheme 9. Alternatively, the double bond can be used to introduce other functionality, such as the hydroxy or fluoro group, as shown in Intermediate Scheme 10. The aldehyde itself may be used to provide the difluoromethyl group at position R3, as shown in Intermediate Scheme 11. The alkene product of the Wittig reaction can undergo numerous other transformations, for example, cyclopropanation, as illustrated in Intermediate Scheme 12. Alternatively, the Wittig reagent may contain a remote functional group, for example, a ketal, as illustrated in Intermediate Scheme 13. This functional group may undergo characteristic functional group transformations after the Wittig/reduction sequence, for example, the hydrolysis of a ketal to a ketone, as illustrated in Intermediate Scheme 13, or the reduction of a ketal to an alcohol as illustrated in Intermediate Scheme 14. In this manner compounds of structural formula I with a variety of different R3 substituents may be obtained. The specific examples given are intended to convey general principles and are not intended to limit the scope of the R3 substituents.
  • Figure US20090181994A1-20090716-C00019
  • Figure US20090181994A1-20090716-C00020
  • Figure US20090181994A1-20090716-C00021
  • Figure US20090181994A1-20090716-C00022
  • Figure US20090181994A1-20090716-C00023
  • Figure US20090181994A1-20090716-C00024
  • Figure US20090181994A1-20090716-C00025
  • General functional group chemical transformations used to prepare compounds of the present invention are illustrated below in the preparation of specific compounds of the present invention.
  • These functional group transformations are of a general variety well understood by those skilled in the art.
  • Figure US20090181994A1-20090716-C00026
    Figure US20090181994A1-20090716-C00027
    Figure US20090181994A1-20090716-C00028
  • The following Examples are provided to illustrate the invention and are not to be construed as limiting the scope of the invention in any manner.
    • EXAMPLE 1
  • Figure US20090181994A1-20090716-C00029
    • 3-Methoxy-4-[4-methyl-5-(4-pentylbicyclo[2.2.2]oct-1-yl)-4H-1,2,4-triazol-3-yl]phenol (1-F)
  • Figure US20090181994A1-20090716-C00030
    • Step A:
  • To a magnetically stirred solution of 4-benzyloxy-2-hydroxybenzonitrile (1-A, WO 00/69841) (7.95 g, 35.3 mmol) and iodomethane (5.43 mL, 87.2 mmol) in DMF (90 mL) cooled to −5° was added all at once sodium hydride (60% dispersion, 2.17 g, 54.2 mmol). The mixture was stirred for 30 min, warmed to room temperature and stirred for an additional 2 h. Most of the DMF was removed in vacuo, and the residue was partitioned between water and ethyl acetate. The aqueous phase was extracted three times with ethyl acetate. The combined organic phases were washed with water and saturated brine and dried (MgSO4). The residue after removal of the solvent in vacuo was triturated with hexane and chromatographed on silica gel with hexanes-CH2Cl2 (2:3) to give 4-benzyloxy-2-methoxybenzonitrile (1-B). MS: m/z 240 (M+1); 1H NMR (500 MHz, CDCl3): δ 7.47 (d, 1H, J=8.4 Hz), 7.36-7.45 (m, 5H), 6.58 (dd, 1H, J=2.3, 8.4 Hz), 6.57 (d, 1H, J=2.3 Hz), 5.10 (s, 2H), 3.88 (s, 3H) ppm.
    • Step B:
  • A vigorously stirred suspension of 4-benzyloxy-2-methoxybenzonitrile (1-B) (1.20 g, 5.0 mmol), sodium azide (732 mg, 11.3 mmol), and triethylamine hydrochloride (1.54 g, 11.3 mmol) in toluene (6 mL) was heated at 110° for 48 h. The brown suspension was cooled, water (15 mL) was added, and the mixture stirred for 30 min. The organic layer was separated and extracted with water (5 mL). The combined aqueous extracts were acidified to about pH 1 with concentrated HC1. The gum that initially precipitated solidified upon stirring for 30 min. The solid was filtered, washed with water, and dried to give 5-[4-(benzyloxy)-2-methoxyphenyl]-2H-tetrazole (1-C). 1H NMR (500 MHz, CDCl3): δ12.9 (vbs, 1H), 7.37 (d, 1H, J=8.7 Hz), 7.34-7.48 (m, 5H), 6.78 (dd, 1H, J=2.3, 8.7 Hz), 6.70 (d, 1H, J=2.3 Hz), 5.15 (s, 2H), 4.05 (s, 3H) ppm.
    • Step C:
  • Oxalyl chloride (3.49 ml, 40 mmol) was added dropwise to a solution of N-methyl-4-pentylbicyclo[2.2.2]octane-1-carboxamide (1-D) (952 mg, 4.0 mmol) in dry CH2Cl2 at room temperature. After the vigorous gas evolution subsided, the solution was stirred at room temperature for 2 h. The CH2Cl2 was removed carefully in vacuo at room temperature and then at 50°. The clear syrupy residue was dissolved in toluene (8 mL) and 5-[4-(benzyloxy)-2-methoxyphenyl]-2H-tetrazole (1-C) (1.13 g, 4.0 mmol) added. The mixture was heated at 120° for 9 h. The mixture was cooled, and the precipitated solid was filtered, washed with toluene and dried to afford the triazole hydrochloride salt. The salt was partitioned between CH2Cl2 and 10% aqueous K2CO3. The aqueous phase was extracted twice with CH2Cl2. The combined CH2Cl2 extracts were dried (MgSO4) and evaporated in vacuo. The residue was chromatographed on silica gel with 5% MeOH/CH2Cl2 to give 3-[4-(benzyloxy)-2-methoxyphenyl]-4-methyl-5-(4-pentylbicyclo[2.2.2]oct-1-yl)-4H-1,2,4-triazole (1-E). MS: m/z 474 (M+1); 1H NMR (500 MHz, CDCl3): δ 7.33-7.47 (m, 6H), 6.65 (dd, 1H, J=2.3, 8.5 Hz), 6.60 (d, 1H, J=2.3 Hz), 5.10 (s, 2H), 3.75 (s, 3H), 3.48 (s, 3H), 2.08 (m, 6H), 1.51 (m, 6H), 1.00-1.35 (m, 8H), 0.89 (t, 3H, J=7.2) ppm.
    • Step D:
  • A solution of 3-[4-(benzyloxy)-2-methoxyphenyl]-4-methyl-5-(4-pentylbicyclo[2.2.2]oct-1-yl)-4H-1,2,4-triazole (1-E) (272 mg, 0.572 mmol) in MeOH (8 mL) was hydrogenated for 19 h with 10% Pd/C catalyst (27 mg) at room temperature and atmospheric pressure. The catalyst was filtered and washed with MeOH. The MeOH was removed in vacuo to afford 3-methoxy-4-[4-methyl-5-(4-pentylbicyclo[2.2.2]oct-1-yl)-4H-1,2,4-triazol-3-yl]phenol (1-F). MS: m/z 384 (M+1); 1H NMR (500 MHz, DMSO-d6): δ 9.94 (s, 1H), 7.09 (d, 1H, J=8.3), 6.53 (d, 1H, J=1.6 Hz), 6.46 (dd, 1H, J=2.2, 8.2 Hz), 3.72 (s, 3H), 3.40 (s, 3H), 1.95 (m, 6H), 1.44 (m, 6H), 1.07-1.33 (m, 8H), 0.86 (t, 3H, J=7.2).
    • EXAMPLE 2
  • Figure US20090181994A1-20090716-C00031
    • 3-Methyl-4-[4-methyl-5-(4-pentylbicyclo[2.2.2]oct-1-yl)-4H-1,2,4-triazol-3-yl]phenol (2-G)
  • Figure US20090181994A1-20090716-C00032
    • Step A:
  • (Trimethylsilyl) diazomethane (2M/hexane, 53 mL, 106 mmol) was added slowly to a solution of 4-pentylbicyclo[2.2.2]octane-1-carboxylic acid (2-A) (20.3 g, 90.6 mmol) in methylene chloride (100 mL) and methanol (40 mL) until the yellow color persisted. After stirring for 10 min at room temperature, the solution was concentrated in vacuo to give methyl 4-pentylbicyclo[2.2.2]octane-1-carboxylate (2-B). 1H NMR (500 MHz, CDCl3): δ 0.89 (t, 3H); 1.20 (m, 8H); 1.39 (m, 6H); 1.77 (m, 6H); 3.65 (s, 3H) ppm.
    • Step B:
  • Hydrazine (anhydrous, 103 mL, 88.7 mmol) was added to a solution of methyl 4-pentylbicyclo[2.2.2]octane-1-carboxylate (2-B) in ethylene glycol (180 mL) and the mixture was stirred under reflux for 17 h. After cooling to room temperature, the mixture was poured into water (1500 mL) and extracted with methylene chloride (3×600 mL). The combined extracts were washed twice with water, brine, dried (MgSO4) and concentrated in vacuo to provide 4-pentylbicyclo[2.2.2]octane-1-carbohydrazide (2-C). 1H NMR (500 MHz, CDCl3): δ 0.90 (t, 3H); 1.21 (m, 8H); 1.43 (m, 6H); 1.74 (m, 6H); 3.85 (broad s, 2H); 6.81 (broad s, 1H) ppm.
    • Step C:
  • 2-Chloro-1,3-dimethyl-4,5-dihydro-1H-imidazol-3-ium chloride (5.07 g, 30.0 mmol) was added to a solution of 2-methyl-4-methoxybenzoic acid (2-D) (856 mg, 5.0 mmol) and 4-pentylbicyclo[2.2.2]octane-1-carbohydrazide (2-C) (1.25 g, 5.25 mmol) in methylene chloride (60 mL) followed by triethylamine (8.36 mL, 60 mmol) and the mixture stirred at room temperature for 48 h. The mixture was diluted with methylene chloride and washed with water, 1N HCl, 10% NaHCO3, brine, dried (MgSO4) and concentrated in vacuo. The residue was purified by column chromatography (silica gel, hexane:ethyl acetate, 9:1) to give 2-(4-methoxy-2-methylphenyl)-5-(4-pentylbicyclo[2.2.2]oct-1-yl)-1,3,4-oxadiazole (2-E) Mass spectrum: 369 (M+1); 1H NMR (500 MHz, CDCl3): δ 0.93 (t, 3H); 1.27 (m, 8H); 1.56 (m, 6H); 2.03 (m, 6H); 2.70 (s, 3H); 3.89 (s, 3H); 6.86 (m, 2H); 7.89 (d, 1H) ppm.
    • Step D:
  • 2-(4-Methoxy-2-methylphenyl)-5-(4-pentylbicyclo[2.2.2]oct-1-yl)-1,3,4-oxadiazole (2-E) (988 mg, 2.68 mmol), methylammonium trifluoroacetate (9.72 g, 67 mmol, prepared by combining equimolar amounts of methylamine and trifluoroacetic acid in ether followed by concentration in vacuo), and methylamine (2M/MeOH, 33 mL, 67 mmol) were stirred together in a glass bomb at 150° C. for 114 h. The mixture was concentrated in vacuo and the residue partitioned with methylene chloride and water. The aqueous phase was extracted with methylene chloride and the combined extracts washed with brine, dried (MgSO4) and concentrated in vacuo. The residue was purified by column chromatography (silica gel, ethyl acetate:hexane, 7:3, then 9:1) to give 3-(4-methoxy-2-methylphenyl)-4-methyl-5-(4-pentylbicyclo[2.2.2]oct-1-yl)-4H-1,2,4-triazole (2-F). Mass spectrum: 382 (M+1); 1H NMR (500 MHz, CDCl3): δ 0.93 (t, 3H); 1.27 (m, 8H); 1.56 (m, 6H); 2.12 (m, 6H); 2.18 (s, 3H); 3.49 (s, 3H); 3.87 (s, 3H); 6.85 (m, 2H); 7.24 (d, 1H) ppm.
    • Step E:
  • Boron tribromide (1M/CH2Cl2, 3.21 mL, 3.21 mmol) was added to a solution of 3-(4-methoxy-2-methylphenyl)-4-methyl-5-(4-pentylbicyclo[2.2.2]oct-1-yl)-4H-1,2,4-triazole (2-F) (410 mg, 1.07 mmol) in methylene chloride (6 mL) at 0° C. The mixture was stirred at room temperature for 2 h. The solution was washed with water, 10% NaHCO3, dried (MgSO4) and concentrated in vacuo. The residue was purified by preparative TLC (silica gel, MeOH:methylene chloride, 5:95) to provide 3-methyl-4-[4-methyl-5-(4-pentylbicyclo[2.2.2]oct-1-yl)-4H-1,2,4-triazol-3-yl]phenol (2-G). Mass spectrum: 393 (M+1); 1H NMR (500 MHz, CDCl3): δ 0.93 (t, 3H); 1.27 (m, 8H); 1.56 (m, 6H); 1.97 (s 3H); 2.12 (m, 6H); 3.50 (s, 3H); 6.65 (m, 2H); 6.98 (d, 1H) ppm.
    • EXAMPLE 3
  • Figure US20090181994A1-20090716-C00033
    • 3-Chloro-4-[4-methyl-5-(4-pentylbicyclo[2.2.2]oct-1-yl)-4H-1,2,4-triazol-3-yl]phenol (3-G)
  • Figure US20090181994A1-20090716-C00034
    • Step A:
  • Oxalyl chloride (505 μL, 5.79 mmol) was added dropwise to a mixture of 4-pentylbicyclo[2.2.2]octane-1-carboxylic acid (3-A) in methylene chloride (10 mL). The solution was stirred at room temperature for 3 h and then concentrated in vacuo to give 4-pentylbicyclo[2.2.2]octane-1-carbonyl chloride (3-B). 1H NMR (500 MHz, CDCl3): δ 0.90 (t, 3H); 1.21 (m, 8H); 1.45 (m, 6H); 1.88 (m, 6H) ppm.
    • Step B:
  • N,N-Diisopropylethylamine (1.44 mL, 11.1 mmol) was added to a mixture of 4-pentylbicyclo[2.2.2]octane-1-carboxylic acid (3-A) (1.09 g, 4.45 mmol) and methylamine hydrochloride (1.5 g, 22.3 mmol) in methylene chloride (10 mL) was added and the mixture stirred at room temperature for 18 h. After diluting with methylene chloride, the mixture was washed with water, brine, dried (MgSO4) and concentrated in vacuo to give N-methyl-4-pentylbicyclo[2.2.2]octane-1-carboxamide (3-C). 1H NMR (500 MHz, CDCl3): δ 0.91 (t, 3H); 1.22 (m, 8H); 1.43 (m, 6H); 1.77 (m, 6H); 2.82 (d, 3H) ppm.
    • Step C:
  • Oxalyl chloride (846 μL, 9.7 mmol) was added dropwise to a solution of N-methyl-4-pentylbicyclo[2.2.2]octane-1-carboxamide (3-C) (230 mg, 0.97 mmol) in methylene chloride (2.0 mL) and the mixture stirred at room temperature for 4 h. The solvent and excess reagent were removed in vacuo to provide N-methyl-4-pentylbicyclo[2.2.2]octane-1-carboximidoyl chloride (3-D). Toluene (1.5 mL) was added followed by 5-(2-chloro-4-methoxyphenyl)-1H-tetrazole (3-E) (204 mg, 0.97 mmol) and the mixture refluxed for 18 h. The reaction was cooled to room temperature and the precipitate was filtered, washed with cold toluene, hexane, dissolved in methylene chloride, dried (MgSO4) and concentrated in vacuo to provide 3-(2-chloro-4-methoxyphenyl)-4-methyl-5-(4-pentylbicyclo[2.2.2]oct-1-yl)-4H-1,2,4-triazole (3-F). Mass spectrum: 402 (M+1); 1H NMR (500 MHz, CDCl3): δ 0.94 (t, 3H); 1.27 (m, 8H); 1.56 (m, 6H); 2.13 (m, 6H); 3.56 (s, 3H); 3.89 (s, 3H); 6.95 (dd, 1H); 7.07 (d, 1H); 7.43 (d, 1H).
    • Step D:
  • Boron tribromide (135 μL, 1.43 mmol) was added dropwise to a solution of 3-(2-chloro-4-methoxyphenyl)-4-methyl-5-(4-pentylbicyclo[2.2.2]oct-1-yl)-4H-1,2,4-triazole (3-F) (287 mg, 0.714 mmol) in methylene chloride (5 mL) at 0° C. The mixture was stirred at room temperature for 2.5 h. The solution was washed with water, 10% NaHCO3, dried (MgSO4) and concentrated in vacuo and the residue purified by column chromatography (silica gel, 5% MeOH/methylene chloride) to provide 3-chloro-4-[4-methyl-5-(4-pentylbicyclo[2.2.2]oct-1-yl)-4H-1,2,4-triazol-3-yl]phenol (3-G). Mass spectrum: 388 (M+1); 1H NMR (500 MHz, CDCl3): δ 0.93 (t, 3H); 1.26 (m, 8H); 1.56 (m, 6H); 2.13 (m, 6H); 3.58 (s, 3H); 6.69 (dd, 1H); 6.92 (d, 1H); 7.09 (d 1H) ppm.
    • EXAMPLE 4
  • Figure US20090181994A1-20090716-C00035
    • 5-(4-{1-Methyl-5-[2-(trifluoromethyl)phenyl]-1-H-1,2,4-triazol-3-yl}bicyclo[2.2.2]oct-1-yl)pentan-2-ol (4-J)
  • Figure US20090181994A1-20090716-C00036
    • Step A:
  • [2-(2-Methyl-1,3-dioxolan-2-yl)ethyl](triphenyl)phosphonium bromide (4-A, Synthesis: 532 (1986)) (5.99 g, 12.7 mmol) was stirred in dry THF (200 mL). Potassium bis(trimethylsilyl)amide (20.4 mL, 2M soln in toluene, 10.2 mmol) was added. The reaction was allowed to stir for 30 min. The reaction mixture was then cooled to −78° C. Methyl 4-formylbicyclo[2.2.2]octane-1-carboxylate was added at −78° C. by cannula. The reaction was allowed to warm to room temperature overnight. The volume was reduced by evaporation of THF in vacuo. 100 mL of water was added. The mixture was then layered with 100 mL of diethyl ether. The ether was extracted and dried (MgSO4). The product (methyl 4-[(1E)-3-(2-methyl-1,3-dioxolan-2-yl)prop-1-enyl]bicyclo [2.2.2]octane-1-carboxylate (4-B)) was purified by flash chromatography on silica gel with 10/90 ethyl acetate-hexane mixture.
    • Step B:
    • Methyl 4-[(1E)-3-(2-methyl-1,3-dioxolan-2-yl)prop-1-enyl]bicyclo [2.2.2]octane-1-carboxylate (4-B) (1.1 g) was stirred in ethanol (75 mL). A spatula tip scoop of 10% Pd on carbon (150 mg) was added. A hydrogen balloon was added and the mixture was stirred under hydrogen atmosphere for 3 h. The palladium-on-carbon was filtered and the ethanol was removed in vacuo to yield methyl 4-[3-(2-methyl-1,3-dioxolan-2-yl)propyl]bicyclo[2.2.2]octane-1-carboxylate (4-C).
    Step C:
  • Methyl 4-[3-(2-methyl-1,3-dioxolan-2-yl)propyl]bicyclo [2.2.2]octane-1-carboxylate (4-C) (1.0 g, 3.38 mmol) was stirred in a solution of 90% methanol and 10% water (50 mL). Excess potassium hydroxide (2.0 g) was added. The mixture was refluxed overnight. The cooled mixture was acidified with 1N hydrochloric acid (100 mL) and then washed twice with ethyl acetate (100 mL). The combined organic layers were dried (MgSO4). Ethyl acetate was removed in vacuo yielding pure 4-[3-(2-methyl-1,3-dioxolan-2-yl)propyl]bicyclo[2.2.2]octane-1-carboxylic acid (4-D).
    • Step D:
  • 4-[3-(2-Methyl-1,3-dioxolan-2-yl)propyl]bicyclo [2.2.2]octane-1-carboxylic acid (4-D) (0.200 g, 0.708 mmol) was combined with 2-(trifluoromethyl)benzoic hydrazide (4-E) (0.173 g, 0.847 mmol) and azeotroped twice from toluene. The mixture was then stirred in dry methylene chloride (10 mL). 2-Chloro-1,3-dimethylimidazolinium chloride (4-F) (0.718 g, 4.25 mmol) was added followed by 1.184 mL of triethylamine. The reaction was allowed to stir for 2 h. The reaction was diluted with methylene chloride and was washed with water. The resulting oxadiazole, 2-{4-[3-(2-methyl-1,3-dioxolan-2-yl)propyl]bicyclo [2.2.2]oct-1-yl}-5-[2-(trifluoromethyl)phenyl]-1,3,4-oxadiazole (4-G) was purified by flash chromatography on silica gel with 50/50 ethyl acetate-hexane mixture.
    • Step E:
  • 2-{4-[3-(2-Methyl-1,3-dioxolan-2-yl)propyl]bicyclo [2.2.2]oct-1-yl}-5-[2-(trifluoromethyl)phenyl]-1,3,4-oxadiazole (4-G) (0.158 g) was stirred in a mixture of 90% acetone/10% water (20 mL). p-Toluenesulfonic acid (10 mg) was added to the solution. The reaction was heated to reflux for 1 h. The volume was reduced by evaporation of acetone in vacuo. The mixture was then layered with ethyl acetate (25 mL) and saturated sodium bicarbonate solution (25 mL). The ethyl acetate layer was extracted and dried (MgSO4). Solvent was removed in vacuo to afford pure 5-(4-{5-[2-(trifluoromethyl)phenyl]-1,3,4-oxadiazol-2-yl}bicyclo[2.2.2]oct-1-yl)pentan-2-one (4-H).
    • Step F:
  • 5-(4-{5-[2-(Trifluoromethyl)phenyl]-1,3,4-oxadiazol-2-yl}bicyclo [2.2.2]oct-1-yl)pentan-2-one (4-H) (0.072 g) was stirred in methanol (2 mL) at 0° C. Sodium borohydride (20 mg) was added. The reaction was allowed to stir to room temperature. The mixture was then layered with ethyl acetate (15 mL) and water (15 mL). The ethyl acetate layer was extracted and dried (MgSO4). Solvent was removed in vacuo to afford pure 5-(4-{5-[2-(trifluoromethyl)phenyl]-1,3,4-oxadiazol-2-yl}bicyclo[2.2.2]oct-1-yl)pentan-2-ol (4-I).
    • Step G:
  • 5-(4-{5-[2-(Trifluoromethyl)phenyl]-1,3,4-oxadiazol-2-yl}bicyclo [2.2.2]oct-1-yl)pentan-2-ol (4-I) (50 mg) was placed in a sealed vial in a solution of 2M methylamine in methanol (2.5 mL). A small spatula scoop of methylamine TFA salt was added and the vial was sealed. The sealed vial was heated to 150° C. for 3 d. The reaction was diluted with ethyl acetate (15 mL), washed with water (15 mL), and dried (MgSO4). Ethyl acetate was removed in vacuo. The product, 5-(4-{1-methyl-5-[2-(trifluoromethyl)phenyl]-1-H-1,2,4-triazol-3-yl}bicyclo [2.2.2]oct-1-yl)pentan-2-ol (4-J), was purified by preparative reverse phase HPLC on a C-18 silica gel column using a gradient of acetonitrile-water buffered with 0.1% trifluoroacetic acid. The effluent containing the pure triazole was made basic with 10% NaHCO3, evaporated in vacuo to remove most of the acetonitrile, and extracted with methylene chloride. The organic extract was dried (MgSO4) and evaporated, and the residue dried under vacuum to provide the desired compound. MS (ESI+)=422.5 (M+1); 1H NMR (500 MHz, CDCl3): δ 1.21 (2H, m), 1.23 (3H, d, J=6.5 Hz), 1.29 (2H, m), 1.57 (6H, m), 2.13 (6H, m), 3.47 (3H, s), 3.85 (1H, m), 7.51 (1H, m), 7.70 (2H, m), 7.85 (1H, m) ppm.
    • EXAMPLE 5
  • Figure US20090181994A1-20090716-C00037
    • 3-Chloro-4-{5-[4-(4-hydroxypentyl)bicyclo[2.2.2]oct-1-yl]-1-methyl-1-H-1,2,4-triazol-3-yl}phenol (5-K)
  • Figure US20090181994A1-20090716-C00038
    • Step A:
  • 4-[3-(2-Methyl-1,3-dioxolan-2-yl)propyl]bicyclo [2.2.2]octane-1-carboxylic acid (4-D) (0.300 g, 1.06 mmol) was combined with 2-chloro-4-methoxybenzohydrazide (5-E) (0.255 g, 1.275 mmol) and azeotroped twice from toluene. The mixture was then stirred in dry methylene chloride (15 mL). 2-Chloro-1,3-dimethylimidazolinium chloride (5-F) (1.075 g, 6.36 mmol) was added followed by 1.77 mL of triethylamine. The reaction was allowed to stir for 2 h. The reaction was diluted with methylene chloride and was washed with water. The resulting oxadiazole, 2-(2-chloro-4-methoxyphenyl)-5-{4-[3-(2-methyl-1,3-dioxolan-2-yl)propyl]bicyclo [2.2.2]oct-1-yl}-1,3,4-oxadiazole (5-G) was purified by flash chromatography on silica gel with 50/50 ethyl acetate-hexane mixture.
    • Step B:
    • 2-(2-Chloro-4-methoxyphenyl)-5-{4-[3-(2-methyl-1,3-dioxolan-2-yl)propyl]bicyclo[2.2.2]oct-1-yl}-1,3,4-oxadiazole (5-G) (0.200 g) was stirred in a mixture of 90% acetone/10% water (20 mL). p-Toluenesulfonic acid (15 mg) was added to the solution. The reaction was heated to reflux for 1 h. The volume was reduced by evaporation of acetone in vacuo. The mixture was then layered with ethyl acetate (25 mL) and saturated sodium bicarbonate solution (25 mL). The ethyl acetate layer was extracted and dried (MgSO4). Solvent was removed in vacuo to afford pure 5-{4-[5-(2-chloro-4-methoxyphenyl)-1,3,4-oxadiazol-2-yl]bicyclo[2.2.2]oct-1-yl}pentan-2-one (5-H).
    Step C:
  • 5-{4-[5-(2-Chloro-4-methoxyphenyl)-1,3,4-oxadiazol-2-yl]bicyclo [2.2.2]oct-1-yl}pentan-2-one (5-H) (0.150 g, 0.373 mmol) was stirred in methanol (5 mL) at 0° C. Sodium borohydride (0.0169 g, 0.448 mmol) was added. The reaction was allowed to stir to room temperature. The mixture was then layered with ethyl acetate (20 mL) and water (20 mL). The ethyl acetate layer was extracted and dried (MgSO4). Solvent was removed in vacuo to afford 5-{4-[5-(2-chloro-4-methoxyphenyl)-1,3,4-oxadiazol-2-yl]bicyclo [2.2.2]oct-1-yl}pentan-2-ol (5-I).
    • Step D:
  • 5-{4-[5-(2-Chloro-4-methoxyphenyl)-1,3,4-oxadiazol-2-yl]bicyclo [2.2.2]oct-1-yl}pentan-2-ol (5-I) (50 mg) was placed in a sealed vial in a solution of 2M methylamine in methanol (2.5 mL). A small spatula scoop of methylamine TFA salt was added and the vial was sealed. The sealed vial was heated to 150° C. for 24 h. The reaction was diluted with ethyl acetate (15 mL), washed with water (15 mL), and dried (MgSO4). Ethyl acetate was removed in vacuo. The product, 5-{4-[5-(2-chloro-4-methoxyphenyl)-1-methyl-1-H-1,2,4-triazol-3-yl]bicyclo[2.2.2]oct-1-yl}pentan-2-ol (5-J), was purified by preparative TLC with 5% methanol/95% ethyl acetate.
    • Step E:
  • 5-{4-[5-(2-Chloro-4-methoxyphenyl)-1-methyl-1-H-1,2,4-triazol-3-yl]bicyclo [2.2.2]oct-1-yl}pentan-2-ol (5-J) (0.036 g, 0.086 mmol) was placed in a small vial with 0.5 mL of DMF. Sodium ethanethiolate (0.0218 g, 0.260 mmol) was added to the solution. The vial was sealed and heated to 100° C. for 1.5 h. The incomplete reaction required another 1.5 equivalents of sodium ethanethiolate (0.011 g). The vial was resealed and heated at 100° C. for 1 h. The product, 3-chloro-4-{5-[4-(4-hydroxypentyl)bicyclo [2.2.2]oct-1-yl]-1-methyl-1-H-1,2,4-triazol-3-yl}phenol (5-K) was purified by preparative reverse phase HPLC on a C-18 silica gel column using a gradient of acetonitrile-water buffered with 0.1% trifluoroacetic acid. The effluent containing the pure triazole was made basic with 10% NaHCO3, evaporated in vacuo to remove most of the acetonitrile, and extracted with methylene chloride. The organic extract was dried (MgSO4) and evaporated, and the residue dried under vacuum to provide the desired compound. MS (ESI+)=404.4 (M+1).
    • EXAMPLE 6
  • Figure US20090181994A1-20090716-C00039
    • 5-{4-[5-(2-chloro-4-hydroxyphenyl)-4-methyl-4H-1,2,4-triazol-3-yl]bicyclo[2.2.2]oct-1-yl}pentan-2-one (6-L)
  • Figure US20090181994A1-20090716-C00040
  • 3-Chloro-4-{5-[4-(4-hydroxypentyl)bicyclo [2.2.2]oct-1-yl]-4-methyl-4H-1,2,4-triazol-3-yl}phenol (5-K) (0.0035 g, 0.00869 mmol) was stirred in 0.5 mL of dry methylene chloride over activated 4 A sieves. N-methylmorpholine N-oxide (0.0015 g, 0.013 mmol) was added. The mixture was allowed to stir under N2 for 15 min. Tetrapropylammonium perruthenate (0.00112 g, 0.00956 mmol) was added and the reaction was allowed to stir for 2 h. The mixture was filtered through celite filtering agent. The product, 5-{4-[5-(2-chloro-4-hydroxyphenyl)-4-methyl-4H-1,2,4-triazol-3-yl]bicyclo [2.2.2]oct-1-yl}pentan-2-one (6-L), was purified by preparative reverse phase HPLC on a C-18 silica gel column using a gradient of acetonitrile-water buffered with 0.1% trifluoroacetic acid. The effluent containing the pure triazole was basified with 10% NaHCO3, evaporated in vacuo to remove most of the acetonitrile, and extracted with methylene chloride. The organic extract was dried (MgSO4) and evaporated, and the residue dried under vacuum to provide the desired compound. MS (ESI+)=402.3 (M+1).
    • EXAMPLE 7
  • Figure US20090181994A1-20090716-C00041
    • 3-(4-Fluorophenyl)-5-[4-[4-methyl-5-[2-(trifluoromethyl)phenyl]-4H-1,2,4-triazol-3-yl]bicyclo[2.2.2]oct-1-yl]-1,2,4-oxadiazole (7-F)q2
  • Figure US20090181994A1-20090716-C00042
    • Step A:
  • To a suspension of 4-(methoxycarbonyl)bicyclo[2.2.2]octane-1-carboxylic acid (7-A) (0.906 g, 4.27 mmol) in dichloromethane (20 mL) was added 1,1′-carbonyldiimidazole (1.04 g, 6.41 mmol). The reaction turned into a clear solution instantly with evolving of gas. After the mixture was stirred at room temperature for 1 h, 4-fluorobenzamidoxime was added (1.98 g, 12.8 mmol). Stirring was continued overnight. The mixture was then concentrated and the residue was refluxed in toluene for 16 h. The mixture was concentrated and the residue was purified by column chromatography using hexane/ethyl acetate as eluent (7/1) to give methyl 4-[3-(4-fluorophenyl)-1,2,4-oxadiazol-5-yl]bicyclo[2.2.2]octane-1-carboxylate acid (7-B) as a white solid. 1H NMR (500 MHz, CDCl3) δ 1.96-1.99 (m, 6H), 2.08-2.14 (m, 6H), 3.71 (s, 3H), 7.16-7.20 (m, 2H), 8.08-8.10 (m, 2H) ppm. ESI-MS m/z (M+H) 349.2.
    • Step B:
  • The ester (7-B) (1.01 g, 3.06 mmol) was treated with KOH (0.52 g, 9.18 mmol) in methanol/water (95/5, 20 mL). After it was heated at 60° C. for 12 h, the reaction mixture was concentrated, diluted with water, extracted twice with ethyl acetate. The aqueous layer was acidified with 1N HC1 aqueous solution and a white solid precipitated out. The solid 4-[3-(4-fluorophenyl)-1,2,4-oxadiazol-5-yl]bicyclo[2.2.2]octane-1-carboxylic acid (7-C) was collected and further dried by co-evaporating with toluene. ESI-MS m/z (M+H) 317.2.
    • Step C:
  • A mixture of the acid (7-C) (138.9 mg, 0.439 mmol) and 2-(trifluoromethyl)benzoic hydrazide (7-D) (89.7 mg, 0.439 mmol) was first co-evaporated with toluene three times. Dichloromethane (7 mL) was added to the mixture as solvent. To the resulting suspension was added 2-chloro-1,3-dimethylimidazolinium chloride (743 mg, 4.39 mmol) followed by triethylamine (1.2 mL, 8.78 mmol). The mixture was allowed to stir at room temperature under nitrogen for 48 h to ensure the completion of the reaction. The reaction mixture was then diluted with dichloromethane, washed with water, 1N HC1, saturated sodium bicarbonate aqueous solution, and lastly brine. The organics were dried over anhydrous sodium sulfate, filtered and concentrated. The residue was purified by column chromatography using hexane/ethyl acetate (3/1) as eluent to give 3-(4-fluorophenyl)-5-(4-{5-[2-(trifluoromethyl)phenyl]-1,3,4-oxadiazol-2-yl}bicyclo [2.2.2]oct-1-yl)-1,2,4-oxadiazole (7-E) as a white solid. 1H NMR (500 MHz, CDCl3) δ 2.25 (s, 12H), 7.21 (t, J=8.7 Hz, 2H), 7.74-7.76 (m, 2H), 7.91 (m, 1H), 8.11-8.15 (m, 3H) ppm. ESI-MS m/z (M+H) 485.2.
    • Step D:
  • A mixture of above 1,2,4-oxadiazole (7-E) (115.2 mg, 0.238 mmol) and the trifluoroacetic acid salt of methylamine (1.73 g, 11.9 mmol) in a 2M solution of methylamine in methanol (4 mL) was heated at 150° C. in a sealed tube for 48 h. The mixture was then concentrated, and the residue was taken up in dichloromethane, washed with saturated sodium bicarbonate aqueous solution. The organics were concentrated and the residue was purified using reverse-phase HPLC with TFA-buffered acetonitrile/water (40-80%) as eluent. The fractions containing the product were combined, neutralized with saturated sodium bicarbonate aqueous solution and lyophilized from acetonitrile/water to provide 3-(4-fluorophenyl)-5-(4-{4-methyl-5-[2-(trifluoromethyl)phenyl]-4H-1,2,4-triazol-3-yl}bicyclo[2.2.2]oct-1-yl)-1,2,4-oxadiazole (7-F). 1HNMR (CDCl3) δ 2.25-2.35 (m, 12H), 3.53 (s, 3H), 7.21 (t, J=8.7 Hz, 2H), 7.54 (m, 1H), 7.73 (m, 2H), 7.88 (m, 1H), 8.13 (m, 2H). ESI-MS m/z (M+H) 498.2.
    • EXAMPLE 8
  • Figure US20090181994A1-20090716-C00043
    • 4-[4-Methyl-5-(4-phenylbicyclo[2.2.2]oct-1-yl)-4H-1,2,4-triazol-3-yl]-3-(trifluoromethyl)phenol (8-F)
  • Figure US20090181994A1-20090716-C00044
  • Preparation of 4-phenylbicyclo[2.2.2]octane-1-carboxylic acid (8-A)
    • LITERATURE REFERENCE
    • Chapman, N. B, Sotheeswaran, S., and Toyne, K. J, J. Org. Chem, 35: 917-923 (1970)
    Step A:
  • To a magnetically stirred solution of 4-phenylbicyclo[2.2.2]octane-1-carboxylic acid (8-A) (70 mg, 0.30 mmol) in methylene chloride (1 mL) at room temperature was added 2 M oxalyl chloride in methylene chloride (0.61 mL, 1.22 mmol). Two drops of catalytic DMF were added to catalyze the reaction. The reaction was stirred for 30 min and solvent and reagent removed in vacuo. Methylene chloride (1 mL) was added to the residue, followed by 4-(benzyloxy)-2-(trifluoromethyl)benzoic hydrazide (8-B) (141 mg, 0.46 mmol) and triethylamine (0.07 mL, 0.46 mmol). The reaction was stirred at room temperature overnight to afford intermediate 8-C, N′-[4-(benzyloxy)-2-(trifluoromethyl)benzoyl]-4-phenylbicyclo[2.2.2]octane-1-carbohydrazide, which was not isolated. To the crude product (8-C) were then added 2-chloro-1,3-dimethylimidazolinium chloride (257 mg, 1.52 mmol), more triethylamine (0.42 mL, 3.04 mmol), and methylene chloride (2 mL). The reaction was stirred at room temperature for 4 h. The reaction mixture was then diluted with methylene chloride (30 mL) and washed with water (30 mL) two times and with brine (30 mL) once. The combined aqueous layers were extracted with methylene chloride (25 mL) once. The combined organic layers were dried (MgSO4) and the solvent removed in vacuo. The residue was chromatographed on silica with 10% ethyl acetate in hexanes as eluant to give 2-[4-(benzyloxy)-2-(trifluoromethyl)phenyl]-5-(4-phenylbicyclo[2.2.2]oct-1-yl)-1,3,4-oxadiazole (8-D). MS: m/z 505 (M+1).
    • Step B:
  • The trifluoroacetate salt of methylamine (380 mg, 2.61 mmol) and 2-[4-(benzyloxy)-2-(trifluoromethyl)phenyl]-5-(4-phenylbicyclo[2.2.2]oct-1-yl)-1,3,4-oxadiazole (8-D) were suspended in a 2 M solution of methylamine in methanol (1.3 mL, 2.61 mmol) and heated at 150° C. overnight. After being cooled to room temperature, the reaction mixture was partitioned between ethyl acetate (25 mL) and saturated aqueous sodium bicarbonate (30 mL). The layers were separated and the aqueous layer extracted with twice with ethyl acetate (25 mL). The combined organic layers were washed with brine, dried (MgSO4), and solvent removed in vacuo. The residue was then dissolved in methanol (8 mL) and purified by reverse phase chromatography using gradient elution with 10% acetonitrile (0.1% TFA)/water (0.1% TFA) to 100% acetonitrile (0.1% TFA) over 10 min (20 mL/min). The fractions containing product were partitioned between saturated aqueous sodium bicarbonate (25 mL) and methylene chloride (15 mL). The layers were separated and the aqueous layer was extracted with methylene chloride (15 mL) three times, dried (MgSO4), and the solvent removed in vacuo to afford 3-[4-(benzyloxy)-2-(trifluoromethyl)phenyl]-4-methyl-5-(4-phenylbicyclo[2.2.2]oct-1-yl)-4H-1,2,4-triazole (8-E). MS: m/z 518 (M+1).
    • Step C:
  • The 3-[4-(Benzyloxy)-2-(trifluoromethyl)phenyl]-4-methyl-5-(4-phenylbicyclo[2.2.2]oct-1-yl)-4H-1,2,4-triazole (8-E) (27 mg, 0.05 mmol) was dissolved in ethyl acetate/methanol (1:1, 4 mL) to which 10% palladium-on-carbon (4 mg) was added. The reaction was then placed under hydrogen atmosphere and stirred for 3 h at room temperature and pressure. After appropriate evacuation of the hydrogen atmosphere, the palladium was filtered through a filter aid with methanol (40 mL). The filtrate was collected and the solvent removed in vacuo to afford 4-[4-methyl-5-(4-phenylbicyclo[2.2.2]oct-1-yl)-4H-1,2,4-triazol-3-yl]-3-(trifluoromethyl)phenol (8-F). MS: m/z 428 (M+1); 1H NMR (500 MHz, CDCl3): δ 1.92 (6H, m), 2.11 (6H, m), 3.41 (3H, s), 7.17 (2H, m), 7.24 (1H, m), 7.31 (2H, m), 7.38 (3H, m) ppm.
    • EXAMPLE 9
  • Figure US20090181994A1-20090716-C00045
    • 3-Chloro-4-[5-(4-ethylbicyclo[2.2.2]oct-1-yl)-4-methyl-4H-1,2,4-triazol-3-yl]phenol (9-E)
  • Figure US20090181994A1-20090716-C00046
    • Step A:
  • To a stirred solution of 4-ethyl-1-carboxylbicyclo[2.2.2]octane (Chapman, N. B. et al. J. Org. Chem., 1970, 35, 917) (45 mg, 0.26 mmol) in 1 mL of degassed DMF were added methylamine (2M in THF, 1 mL, 2 mmol), triethylamine (0.075 mL, 0.53 mmol) and TFFH (70 mg, 0.26 mmol). The solution was stirred at room temperature for 1 h, then diluted with 20 mL of ethyl acetate and washed with 1N aqueous HCl and brine. The organic layer was dried over anhydrous sodium sulfate and evaporated. The brown oily residue was loaded onto a flash silica gel column and eluted with a gradient ranging from 10 to 40% of ethyl acetate in hexanes. 4-Ethyl-N-methylbicyclo[2.2.2]octane-1-carboxamide (9-B) was isolated as a clear, colorless oil.
  • 1H NMR (500 MHz, CDCl3): δ 0.80 (3H, t, J=7.2 Hz), 1.18 (2H, q, J=7.2 Hz), 1.42 (6H, m), 1.76 (6H, m), 2.81 (3H, d, J=6.1 Hz).
    • Step B:
  • To a stirred solution of 9-B (45 mg, 0.23 mmol) in 0.25 mL of dry CH2Cl2 was added oxalyl chloride (2M in CH2Cl2, 0.29 mL, 0.58 mmol) and 1 drop of dry DMF. The solution was stirred at room temperature for 2 h, then evaporated. The yellow residue was redissolved in dry toluene and 5-(2-chloro-4-methoxyphenyl)-2H-tetrazole (9-C) was added. The reaction mixture was heated to reflux under inert atmosphere and stirred for additional 1.5 h before being cooled down to room temperature. The solid was filtered, washed with toluene, then redissolved in methylene chloride and washed with saturated aqueous sodium bicarbonate and brine solution. The organic layer was dried, then evaporated. The yellowish residue was purified on a short plug of flash silica gel, eluting with a gradient ranging from 0% to 3% of methanol in methylene chloride. 3-(2-Chloro-4-methoxyphenyl)-5-(4-ethylbicyclo[2.2.2]oct-1-yl)-4-methyl-4H-1,2,4-triazole (9-D) was isolated as a white powder. MS (ESI+)=360.3 (M+1); 1H NMR (500 MHz, CDCl3): δ 0.82 (3H, t, J=7.0 Hz), 1.22 (2H, q, J=7.0 Hz), 1.52 (6H, m), 2.10 (6H, m), 3.55 (3H, s), 3.88 (3H, s), 6.92 (1H, dd, J=8.4 Hz, J=2.8 Hz), 7.04 (1H, d, J=2.4 Hz), 7.41 (1H, d, J=8.4 Hz).
    • Step C:
  • Triazole 9-D (30 mg, 0.08 mmol) was dissolved in 0.5 mL of dry methylene chloride, placed under an inert atmosphere, and cooled to 0° C. To this solution was added BBr3 (1 M in CH2Cl2, 0.25 mL, 0.25 mmol) and the cooling bath was immediately removed. The reaction was stirred for 2 h then diluted with 20 mL of methylene chloride and washed with 1 N aqueous NaOH and brine. The residue was chromatographed by reverse-phase HPLC, eluting with a gradient of 0 to 100% acetonitrile in water. The product, 3-chloro-4-[5-(4-ethylbicyclo[2.2.2]oct-1-yl)-4-methyl-4H-1,2,4-triazol-3-yl]phenol (9-E), was isolated as a white powder. MS (ESI+)=346.2 (M+1); 1H NMR (500 MHz, CDCl3): δ 0.85 (3H, t, J=7.5 Hz), 1.25 (2H, q, J=7.5 Hz), 1.55 (6H, m), 2.13 (6H, m), 3.58 (3H, s), 6.68 (1H, dd, J=8.4 Hz, J=2.6 Hz), 6.91 (1H, d, J=2.6 Hz), 7.10 (1H, d, J=8.4 Hz).
    • EXAMPLE 10
  • Figure US20090181994A1-20090716-C00047
    • 3-{4-[2-(Ethylsulfonyl)ethyl]bicyclo[2.2.2]oct-1-yl}-4-methyl-5-[2-(trifluoromethyl)phenyl]-4H-1,2,4-triazole (10-6)
  • Figure US20090181994A1-20090716-C00048
    • Step A:
  • Diethyl (ethylsulfonomethane)phosphonate (1.12 g, 4.6 mmol) (Popoff, I. C. et al. J. Org. Chem. 34: 1128-30 (1969)) and 4-carbomethoxybicyclo[2.2.2]octane-1-carboxaldehyde (10-1) (0.82 g, 4.2 mmol) (Adcock, W., Kok, G. B. J. Org. Chem. 50: 1079-1087 (1985)) were dissolved in 8 mL of absolute methanol. The mixture was placed under nitrogen atmosphere, cooled in an ice-bath, and treated with 0.5M solution of sodium methoxide in methanol (8.8 mL, 4.4 mmol). The reaction mixture was kept under reflux for 4 h, then cooled to room temperature, concentrated under diminished pressure, then treated with 2 mL of water and allowed to sit in the refrigerator overnight. The mixture was filtered and the solid washed with a small amount of cold 1:1 MeOH/water. The resulting white solid was collected and dried under vacuum to give the unsaturated sulfone 10-2. MS (ESI+)=287 (M+1).
    • Step B:
  • Sulfone 10-2 (880 mg, 3.08 mmol) was dissolved in a 1:2 mixture of ethyl acetate/methanol (30 mL), placed under nitrogen atmosphere, then treated with 10% Pd/C (800 mg). The reaction was placed under hydrogen atmosphere and stirred vigorously for 90 min. The resulting solution was filtered through celite, washed with methanol and ethyl acetate and evaporated to give methyl 4-[2-(ethylsulfonyl)ethyl]bicyclo[2.2.2]octane-1-carboxylate (10-3) as a white solid.
    • Step C:
  • Ester 10-3 (880 mg, 3 mmol) was dissolved in 10% water/methanol solution (100 mL) and treated with 1 g of potassium hydroxide. The reaction was heated at 60° C. for 1 h then at 45° C. overnight. The mixture was concentrated in vacuo then acidified to pH 2 with 1M HCl and extracted with three portions of methylene chloride. The organic layers were combined, dried over anhydrous sodium sulfate and evaporated to give 4-[2-(ethylsulfonyl)ethyl]bicyclo[2.2.2]octane-1-carboxylic acid (10-4).
    • Step D:
  • Carboxylic acid 10-4 (810 mg, 2.96 mmol) was dissolved in 12 mL of anhydrous methylene chloride under nitrogen atmosphere, treated with oxalyl chloride (2M in methylene chloride, 4.4 mL, 8.8 mmol) and subsequently with 5 drops of DMF. The reaction was stirred at room temperature under nitrogen atmosphere for 90 min, then evaporated and placed under vacuum for 20 min. The acid chloride was dissolved in anhydrous methylene chloride (12 mL), cooled in an ice-bath, and then treated dropwise with a solution of methylamine (2M in THF, 8.9 mL, 17.8 mmol). Upon addition of the amine, the cooling bath was removed and the reaction stirred at ambient temperature for 30 min. The mixture was diluted with 200 mL of methylene chloride and washed with 1N aqueous HCl, saturated aqueous sodium bicarbonate, and brine. The organic layer was dried over anhydrous sodium sulfate and evaporated. The residue was subjected to chromatography on silica gel eluting with a gradient from 0 to 3.5% methanol in methylene chloride to give 4-[2-(ethylsulfonyl)ethyl]-N-methylbicyclo[2.2.2]octane-1-carboxamide 10-5 as a white powder. MS (ESI+)=288 (M+1).
    • Step E:
  • Methyl amide 10-5 (220 mg, 0.77 mmol) was dissolved in anhydrous methylene chloride (2 mL) and treated with oxalyl chloride (2M in methylene chloride, 0.77 mL, 1.54 mmol) and DMF (2 drops). The solution was stirred at room temperature for 1 h, then solvent removed by evaporation under diminished pressure. The residue was redissolved in anhydrous toluene (2 mL) and treated with 5 [2-(trifluoromethyl)phenyl]1H-tetrazole (214 mg, 1 mmol). The mixture was refluxed for 18 h. The reaction was cooled to room temperature and the cream-colored precipitate was filtered and washed to give 300 mg of crude product as the HCl salt. The salt was taken up in methylene chloride/1N HCl and the aqueous layer was washed with two additional portions of methylene chloride. The organic layers were combined and evaporated and the residue was chromatographed by flash silica gel chromatography. Elution was carried out with a gradient ranging from 0 to 5% methanol/methylene chloride. The appropriate fractions were combined and evaporated to give 3-{4-[2-(ethylsulfonyl)ethyl]bicyclo[2.2.2]oct-1-yl}-4-methyl-5-[2-(trifluoromethyl)phenyl]-4H-1,2,4-triazole (10-6) as a white powder.
  • MS (ESI+)=456.2 (M+1); 1H NMR (500 MHz, CDCl3): δ 1.46 (3H, t, J=7.3 Hz), 1.63 (6H, m), 1.78 (2H, m), 2.19 (6H, m), 2.96 (2H, m), 3.05 (2H, q, J=7.2 Hz), 3.50 (3H, s), 7.56 (1H, m), 7.72 (2H, m), 7.87 (1H, m) ppm.
    • EXAMPLE 11
  • Figure US20090181994A1-20090716-C00049
    • 3-{4-[3-(Ethylsulfonyl)propyl]bicyclo[2.2.2]oct-1-yl}-4-methyl-5-[2-(trifluoromethyl)phenyl]-4H-1,2,4-triazole (11-10)
  • Figure US20090181994A1-20090716-C00050
    • Step A:
  • (Benzyloxycarbonylmethyl)triphenylphosphonium bromide (4.6 g, 9.4 mmol) was azeotroped twice from toluene, and then suspended in 30 mL dry THF. Potassium hexamethyldisilazide (0.5 M in toluene, 16.8 mL, 8.4 mmol) was added dropwise at room temperature and the yellow solution was allowed to stir for 1 h, after which time it became milky white. A solution of 4-carbomethoxybicyclo[2.2.2]octane-1-carboxaldehyde (11-1) (0.50 g, 2.55 mmol) (Adcock, W., Kok, G. B. J. Org. Chem. 50: 1079-1087 (1985)) and benzoic acid (0.015 g, 0.13 mmol) in 2 mL of dry THF was prepared and added dropwise by syringe at room temperature. The mixture was heated to 90° C. and allowed to stir at reflux temperature, after which time the mixture was diluted with 200 mL of ethyl acetate and washed consecutively with 50 mL portions of 1 N HCl (twice), saturated aq. sodium bicarbonate, and brine. The organic layer was dried using magnesium sulfate, and the solvent was removed under reduced pressure. The residue was chromatographed on silica, eluting with a gradient of 5% to 10% ethyl acetate in hexane to provide methyl 4-[(1E)-3-(benzyloxy)-3-oxoprop-1-en-1-yl]bicyclo[2.2.2]octane-1-carboxylate (11-2) as a colorless oil. 1H NMR (500 MHz, CDCl3): δ 7.4 (5H, m), 6.94 (1H, d, J=17 Hz), 5.77 (1H, d, J=17 Hz), 5.21 (2H, s), 3.69 (3H, s), 1.86 (6H, m), 1.63 (6H, m) ppm.
    • Step B:
  • Diester 11-2 (0.625 g, 1.90 mmol) was dissolved in a 1:1 mixture of ethyl acetate/methanol (30 mL), placed under nitrogen atmosphere, then treated with 10% Pd/C (500 mg) and 0.1 mL of acetic acid. The reaction was placed under hydrogen atmosphere and stirred vigorously for 2 hr. The resulting solution was filtered through celite and the solvent was removed under reduced pressure. The residue was partitioned between 200 mL of ethyl acetate and 200 mL of 1 N NaOH solution. The aqueous layer was separated and neutralized, then extracted three times with 50 mL of methylene chloride. The combined organic layers were dried over magnesium sulfate and the solvent was removed under reduced pressure to afford 3-[4-(methoxycarbonyl)bicyclo[2.2.2]oct-1-yl]propanoic acid (11-3). 1H NMR (500 MHz, CDCl3): δ 3.62 (3H, s), 2.20 (2H, broad t, J=9 Hz), 1.75 (6H, m), 1.47 (2H, broad t, J=9 Hz), 1.38 (6H, m) ppm.
    • Step C:
  • Carboxylic acid 11-3 (400 mg, 1.67 mmol) was dissolved in tetrahydrofuran (5 mL) and borane (1 M solution in THF, 2.17 mL, 1.3 eq.) was added dropwise at room temperature. After 2 h the reaction was added to 50 mL of 1 N HCl and then extracted three times with 50 mL of methylene chloride. The combined organic layers were dried over magnesium sulfate and the solvent was removed under reduced pressure to afford crude methyl 4-(3-hydroxypropyl)bicyclo [2.2.2]octane-1-carboxylate (11-4) which was used without purification in the next step. 1H NMR (500 MHz, CD3OD): δ 3.66 (3H, s), 3.62 (2H, t, J=6.5 Hz), 1.78 (6H, m), 1.50 (2H, m), 1.41 (2H, m), 1.17 (2H, m) ppm.
    • Step D:
  • Hydroxyester 11-4 (430 mg, 1.9 mmol) was dissolved in 2.5 mL of anhydrous methylene chloride under nitrogen atmosphere, treated with pyridine (0.5 mL) and methanesulfonyl chloride (0.368 mL, 4.8 mmol) and stirred for 4 h at room temperature. The mixture was diluted with 100 mL of ethyl acetate and washed with 1N aqueous HC1, saturated aqueous sodium bicarbonate, and brine. The organic layer was dried over anhydrous sodium sulfate and evaporated. The crude methyl 4-{3-[(methylsulfonyl)oxy]propyl}bicyclo-[2.2.2]octane-1-carboxylate (11-5) thus afforded was used without purification in the next reaction. 1H NMR (500 MHz, CDCl3): δ 4.22 (2H, t, J=7.5 Hz), 3.68 (3H, s), 3.04 (3H, s), 1.82 (6H, m), 1.70 (2H, m), 1.44 (6H, m), 1.24 (2H, m) ppm.
    • Step E:
  • Mesylate 11-5 (3.30 g, 10.9 mmol) was dissolved in DMF (20 mL) and treated with sodium ethanethiolate (1.82 g, 21.7 mmol). The solution was stirred at 45° C. for 3 h, then the mixture was diluted with 100 mL of ethyl acetate and washed twice with 1N aqueous HC1, then with saturated aqueous sodium bicarbonate, and brine. The organic layer was dried over anhydrous sodium sulfate and evaporated to afford methyl 4-[3-(ethylthio)propyl]bicyclo[2.2.2]octane-1-carboxylate (11-6) as a crude oil which was used without purification in the next step.
  • 1H NMR (500 MHz, CDCl3): δ 3.68 ppm (3H, s), 2.56 (2H, q, J=7 Hz), 2.51 (2H, t, J=7.5 Hz), 1.80 (6H, m), 1.52 (2H, m), 1.42 (6H, m), 1.28 (2H, t, J=7 Hz), 1.02 (2H, m).
    • Step F:
  • Sulfide 11-6 (3.0 g, 11 mmol) was dissolved in methylene chloride (50 mL) and treated with m-chloroperbenzoic acid (75%, 6.2 g). The solution was stirred at room temperature for 2 h, then the mixture was diluted with 100 mL of methylene chloride and washed with saturated aqueous sodium bicarbonate, then twice with saturated aqueous sodium bisulfite, then twice with saturated aqueous sodium bicarbonate, and brine. The organic layer was dried over anhydrous sodium sulfate and evaporated to afford methyl 4-[3-(ethylsulfonyl)propyl]bicyclo[2.2.2]octane-1-carboxylate (11-7) as a crude oil which was used without purification in the next step. 1H NMR (500 MHz, CDCl3): δ 3.68 ppm (3H, s), 2.56 (2H, q, J=7 Hz), 2.51 (2H, t, J=7.5 Hz), 1.80 (6H, m), 1.52 (2H, m), 1.42 (6H, m), 1.28 (2H, t, J=7 Hz), 1.02 (2H, m) ppm.
    • Step G:
  • Sulfone 11-7 (3.1 g, 10 mmol) was dissolved in 9:1 MeOH/water (50 mL) and treated with potassium hydroxide (3 g). The solution was stirred at room temperature overnight, then the mixture was acidified with 1 N HCl and extracted four times with 50 mL of methylene chloride. The organic layer was dried over anhydrous sodium sulfate and evaporated to afford 4-[3-(ethylsulfonyl)propyl]bicyclo[2.2.2]octane-1-carboxylic acid (11-8) which was used without purification in the next step. 1H NMR (500 MHz, CDCl3): δ 3.03 (2H, q, J=7 Hz), 2.94 (2H, dd, J=7.5 Hz), 1.84 (8H, m), 1.45 (8H, m), 1.30 (2H, m) ppm.
    • Step H:
  • Carboxylic acid 11-8 (3.0 g, 11 mmol) was dissolved in 50 mL of anhydrous methylene chloride under nitrogen atmosphere, treated with oxalyl chloride (2 M in methylene chloride, 16.2 mL, 32.4 mmol) and subsequently with 5 drops of DMF. The reaction was stirred at room temperature under nitrogen atmosphere for 90 min, then evaporated and placed under vacuum for 20 min. The acid chloride was dissolved in anhydrous methylene chloride (12 mL), cooled in an ice-bath, and then treated dropwise with a solution of methylamine (2M in THF, 27 mL, 54 mmol). Upon addition of the methylamine, the cooling bath was removed and the reaction stirred at ambient temperature for 30 min. The mixture was diluted with 200 mL of methylene chloride and washed with 1N aqueous HC1, saturated aqueous sodium bicarbonate, and brine. The organic layer was dried over anhydrous sodium sulfate and evaporated. The residue was subjected to chromatography on silica gel eluting with a gradient from 0 to 3% methanol in ethyl acetate to give 4-[3-(ethylsulfonyl)propyl]-N-methylbicyclo[2.2.2]octane-1-carboxamide 11-9 as a white powder. MS (ESI+)=302 (M+1).
  • 1H NMR (500 MHz, CDCl3): δ 5.56 (1H, br s), 3.02 (2H, q, J=7 Hz), 2.94 (2H, dd, J=7.5 Hz), 2.82 (3H, d, J=4 Hz), 1.80 (8H, m), 1.45 (9H, m), 1,28 (2H, m) ppm.
    • Step I:
  • Methyl amide 11-9 (0.470 g, 1.56 mmol) was dissolved in anhydrous methylene chloride (5 mL) and treated with oxalyl chloride (2M in methylene chloride, 1.56 mL, 3.12 mmol) and DMF (2 drops). The solution was stirred at room temperature for 1 h, then solvent removed by evaporation under reduced pressure. The residue was redissolved in anhydrous toluene (7 mL) and treated with 5 [2-(trifluoromethyl)phenyl]1H-tetrazole (368 mg, 1.72 mmol). The mixture was refluxed for 18 h. The reaction was cooled to room temperature and the precipitate was filtered and washed to give 300 mg of crude product as the HCl salt. The salt was taken up in methylene chloride/1N HCl and the aqueous layer was washed with two additional portions of methylene chloride. The organic layers were combined and evaporated and the residue was chromatographed by flash silica gel chromatography. Elution was carried out with a gradient ranging from 0 to 5% methanol/methylene chloride. The appropriate fractions were combined and evaporated to give 3-{4-[3-(ethylsulfonyl)propyl]bicyclo[2.2.2]oct-1-yl}-4-methyl-5-[2-(trifluoromethyl)phenyl]-4H-1,2,4-triazole (11-10) as a white powder.
  • MS (ESI)=470.4 (M+1). 1H NMR (500 MHz, CDCl3): δ 7.87 (1H, m), 7.72 (2H, m), 7.56 (1H, m), 3.49 (3H, s), 3.05 (2H, q, J=7.2 Hz), 2.96 (2H, m), 2.18 (6H, m), 1.86 (2H, m), 1.62 (6H, m), 1.46 (3H, t, J=7.3 Hz), 1.36 (2H, m) ppm.
    • EXAMPLE 12
  • Figure US20090181994A1-20090716-C00051
    • 4-Methyl-3-{-4-[4-(methylsulfonyl)phenyl]bicyclo[2.2.2]oct-1-yl}-5-[2-(trifluoromethyl)phenyl]-4H-1,2,4-triazole (12-G)
  • Figure US20090181994A1-20090716-C00052
    • Step A:
  • To a stirred solution of methyl 4-phenylbicyclo[2.2.2]octane-1-carboxylate 12-A (Chapman, N. B. et al. J. Org. Chem., 1970, 35, 917) (4.80 g, 19.6 mmol) in 1,2-dichloroethane (2 ml, 1 M) was added methanesulfonyl fluoride (4.05 ml, 58.9 mmol) followed by aluminum trichloride (9.17 g, 68.8 mmol). The reaction mixture was stirred overnight under nitrogen atmosphere at ambient temperature followed by addition of another portion of methanesulfonyl fluoride (4.05 ml, 58.9 mmol) and aluminum trichloride (9.17 g, 68.8 mmol). The resulting mixture was heated at 80° C. for 3 h, then cooled to room temperature and diluted with 300 ml of dichloromethane and 200 ml water. The layers were separated and the aqueous layer was washed with two 100 ml portions of dichloromethane. The organic layers were combined, washed with brine, dried (MgSO4), and concentrated in vacuo. The crude product was chromatographed on normal phase flash silica gel column, eluting with a gradient 10-50% EtOAc/hexanes to yield 1.4 g of 12-B (>95% pure). The material was recrystallized from EtOAc to yield compound 12-B.
  • 1H NMR (500 MHz, CDCl3): δ 1.93 (6H, m), 1.99 (6H, m), 3.08 (3H, s), 3.73 (3H, s), 7.55 (2H, d, J=8.3 Hz), 7.90 (2H, d, J=8.1 Hz) ppm.
    • Step B:
  • Carboxylic acid 12-C was prepared in quantitative yield by hydrolysis of ester 12-B (1.1 g, 3.4 mmol) using the procedures described in Example 11, Step G. 1H NMR (500 MHz, CDCl3): δ 1.98 (6H, m), 2.04 (6H, m), 3.11 (3H, s), 7.58 (2H, d, J=7.8 Hz), 7.92 (2H, d, J=7.9 Hz) ppm.
    • Step C:
  • Carboxylic acid 12-C (0.99 g, 3.2 mmol) was converted to hydrazide 12-D using hydrazine (0.124 ml, 4 mmol) and the standard coupling procedure analogous to Example 9, step A. Crude product was purified by flash silica gel chromatography eluting with 0-2% MeOH/CH2Cl2 gradient to yield a white powder. MS (ESI+)=323.2 (M+1).
    • Step D:
  • To a suspension of 12-D (0.67 g, 2.1 mmol) in EtOH (11 ml) was added aldehyde 12-E (0.36 g, 2.1 mmol) and the mixture was refluxed for 18 h. The solvent was removed in vacuo and the solid residue was heated in thionyl chloride (2.9 ml, 40 mmol) for 2 h at 75° C. then stripped to dryness. This residue was treated with methylamine (2M THF, 2 ml) and methylamine (40% aqueous, 1 ml) for 18 h at 70° C. The volatiles were removed in vacuo and the solid was chromatographed on a flash silica gel column using a 10-25% acetone/hexanes gradient to yield compound 12-F. MS (ESI+)=492.3 (M+1); 1H NMR (500 MHz, CDCl3) (2 isomers ratio 3:2): major isomer: δ 2.00 (6H, m), 2.14 (6H, m), 3.10 (3H, s), 3.28 (3H, d, J=5.1 Hz), 5.71 (1H, br. s), 7.47 (1H, m), 7.59 (3H, m), 7.72 (1H, d, J=7.9 Hz), 7.92 (2H, m), 8.26 (1H, d, J=7.9 Hz), 8.70 (1H, br. s) ppm; minor isomer: δ 2.00 (6H, m), 2.32 (6H, m), 2.98 (3H, d, J=4.7 Hz), 3.10 (3H, s), 4.70 (1H, br. s), 7.47 (1H, m), 7.59 (4H, m), 7.92 (2H, m), 8.30 (1H, d, J=7.8 Hz), 8.56 (1H, br. s) ppm.
    • Step E:
  • A solution of 12-F (0.58 g, 1.2 mmol) in EtOH (5 ml) was heated to 40° C. then treated with a solution of ferric chloride (0.4 g, 2.4 mmol) in water (1 ml). The resulting mixture was heated at 90° C. for 18 h. Another portion of ferric chloride (0.4 g, 2.4 mmol) was added and the reaction heated at 90° C. for 24 h. The volatiles were removed in vacuo and the solid was redissolved in CH2Cl2 and washed with a saturated aqueous solution of EDTA and brine then dried (MgSO4) and stripped. The crude product was purified and isolated using the conditions described for purification of 4-J (Example 4, step G) to yield compound 12-G.
  • MS (ESI+)=490.3 (M+1); 1H NMR (500 MHz, CDCl3): δ 2.06 (6H, m), 2.31 (6H, m), 3.08 (3H, s), 3.52 (3H, s), 7.52 (1H, m), 7.59 (2H, d, J=8.4 Hz), 7.71 (2H, m), 7.86 (1H, m), 7.92 (2H, d, J=8.6 Hz) ppm.
    • EXAMPLE 13
  • Figure US20090181994A1-20090716-C00053
    • 3-(4-{4-Methyl-5-[2-(trifluoromethyl)phenyl]-4H-1,2,4-triazol-3-yl}bicyclo [2.2.2]oct-1-yl)-5-(3,3,3-trifluoropropyl)-1,2,4-oxadiazole (13-F)
  • Figure US20090181994A1-20090716-C00054
    • Step A:
  • 4-(Methoxycarbonyl)bicyclo[2.2.2]octane-1-carboxylic acid 13-A (Chapman, N. B. et al. J. Org. Chem., 1970, 35, 917) (4.0 g, 18.9 mmol) was converted to methyl 4-[(methylamino)carbonyl]bicyclo[2.2.2]octane-1-carboxylate 13-B using the methods described in Example 10, steps C and D. Product was purified by flash silica gel chromatography, eluting with 0-5% MeOH/CH2Cl2 gradient to yield a white solid. MS (ESI+)=226.2 (M+1).
    • Step B:
  • Methyl 4-[(methylamino)carbonyl]bicyclo[2.2.2]octane-1-carboxylate 13-B (2.76 g, 12.3 mmol) was converted to 1, 2, 4-triazole 13-C using the procedures described in Example 10, Step E. The product, which precipitated out of reaction mixture as the HCl salt, was dissolved in CH2Cl2, washed twice with saturated aqueous sodium bicarbonate solution, dried (MgSO4) and stripped to yield a white solid. MS (ESI+)=394.2 (M+1);
  • 1H NMR (500 MHz, CDCl3): δ 2.00 (6H, m), 2.18 (6H, m), 3.48 (3H, s), 3.72 (3H, s), 7.51 (1H, m), 7.71 (2H, m), 7.85 (1H, m) ppm.
    • Step C:
  • A solution of methyl ester 13-C (1.19 g, 3.0 mmol) in 5% H2O/MeOH (30 ml) was treated with KOH (0.51 g, 9.0 mmol) at 60° C. under nitrogen atmosphere for 18 h. The resulting mixture was concentrated down, diluted with water (150 ml), washed with EtOAc and acidified with aqueous HCl (1 N) to pH=3. The precipitate was filtered, washed with a small amount of water and ether and dried under vacuum to yield a pink solid (0.87 g, 76%). A portion of the solid (0.67 g, 1.77 mmol) was suspended in CH2Cl2 (15 ml) and treated with carbonyldiimidazole (0.57 g, 3.54 mmol) at room temperature and nitrogen atmosphere. After 2 h, concentrated ammonium hydroxide was added (40 ml) and the reaction was stirred for 18 h. The crude mixture was diluted with water (150 ml) and extracted with 3 portions of CH2Cl2 (70 ml). The organic washes were combined, washed with brine, dried (Na2SO4), and stripped to yield compound 13-D as a white powder. MS (ESI+)=379.3 (M+1).
    • Step D:
  • A solution of carboxamide 13-D (0.64 g, 1.7 mmol) and cyanuric chloride (0.47 g, 2.53 mmol) in DMF (15 ml) was stirred at room temperature under nitrogen atmosphere. After 2 h, DMF was removed in vacuo and the solid was redissolved in CH2Cl2 (100 ml) and washed with saturated aqueous sodium bicarbonate and brine, dried (Na2SO4), and stripped to give the nitrile 13-E as a pale yellow solid. MS (ESI+)=361.3 (M+1); 1H NMR (500 MHz, CDCl3): δ 2.15 (6H, m), 2.22 (6H, m), 3.47 (3H, s), 7.51 (1H, m), 7.72 (2H, m), 7.87 (1H, m) ppm.
    • Step E:
  • A solution of nitrile 13-E (0.56 g, 1.6 mmol) and hydroxylamine (50% aqueous, 4 ml) in ethanol (40 ml) was heated at 80° C. for 18 h. The resulting mixture was cooled to room temperature and concentrated in vacuo. The solid was suspended in toluene, the solvent removed in vacuo, and the solid was dried under reduced pressure. A portion of the resulting white powder (0.050 g, 0.13 mmol) was added to a pre-stirred solution of 4,4,4-trifluorobutyric acid (0.072 g, 0.51 mmol) and carbonyldiimidazole (0.082 g, 0.51 mmol) in CH2Cl2 (3 ml). The resulting mixture was stirred at room temperature for 48 h, then concentrated down. The solid was resuspended in toluene and refluxed under nitrogen atmosphere for 3 h. The crude product was purified and isolated using the conditions described for purification of 4-J (Example 4, step G) to yield 13-F as a white powder.
  • MS (ESI+)=500.2 (M+1); 1H NMR (500 MHz, CDCl3): δ 2.12 (6H, m), 2.30 (6H, m), 2.73 (2H, m), 3.18 (2H, m), 3.54 (3H, s), 7.61 (1H, m), 7.74 (2H, m), 7.87 (1H, m) ppm.
    • EXAMPLE 14
  • Figure US20090181994A1-20090716-C00055
    • 3-(4-{-4-Methyl-5-[2-(trifluoromethyl)phenyl]-4H-1,2,4-triazol-3-yl}bicyclo [2.2.2]oct-1-yl)-5-(3,3,3-trifluoroethyl)-1,2,4-oxadiazole (14-B)
  • Figure US20090181994A1-20090716-C00056
    • Step A:
  • Triazole 14-B was prepared from nitrile 13-E (0.053 g, 0.14 mmol) and 3,3,3-trifluoromethylpropionic acid (0.036 ml, 0.41 mmol) using the method described in Example 13, step E. 3-(4-{4-Methyl-5-[2-(trifluoromethyl)phenyl]-4H-1,2,4-triazol-3-yl}bicyclo [2.2.2]oct-1-yl)-5-(3,3,3-trifluoroethyl)-1,2,4-oxadiazole (14-B) was isolated as a white powder. MS (ESI+)=486.2 (M+1); 1H NMR (500 MHz, CDCl3): δ 2.14 (6H, m), 2.31 (6H, m), 3.53 (3H, s), 3.81 (2H, q, J=9.5 Hz), 7.57 (1H, m), 7.73 (2H, m), 7.87 (1H, m) ppm.
    • EXAMPLE 15
  • Figure US20090181994A1-20090716-C00057
    • 4-Methyl-3-[2-(trifluoromethyl)phenyl]-5-(4-{2-[(trifluoromethyl)sulfonyl]ethyl}bicyclo[2.2.2]oct-1-yl)-4H-1,2,4-triazole (15-G)
  • Figure US20090181994A1-20090716-C00058
    • Step A:
  • To a stirred solution of methyltriphenylphosphonium bromide (9.1 g, 12.8 mmol) in THF (50 ml) at 0° C. was added potassium hexamethyldisilazide (0.5M in toluene, 48.6 ml), dropwise over 5 min. The resulting mixture was allowed to warm up to room temperature over 1 h, then cooled again to 0° C. and treated with methyl 4-formylbicyclo[2.2.2]octane-1-carboxylate 15-A (Chapman, N. B. et al. J. Org. Chem., 1970, 35, 917) (2.5 g, 12.8 mmol). The reaction mixture was stirred at room temperature for 18 h then diluted with EtOAc (350 ml). The organic phase was washed with aqueous HCl (1 N), saturated aqueous sodium bicarbonate, and brine, then dried (Na2SO4) and concentrated in vacuo. The resulting solid was purified by flash silica gel chromatography, eluting with a gradient 0-4% EtOAc/hexanes. The resulting methyl 4-vinylbicyclo[2.2.2]octane-1-carboxylate 15-B was isolated as a clear, colorless oil.
    • Step B:
  • To a stirred solution of olefin 15-B (1.6 g, 8.3 mmol) in THF (20 ml) was added 9-BBN (0.5M in THF, 49 ml), dropwise. The solution was allowed to stir at room temperature for 18 h, then treated sequentially with ethanol (14.5 ml), aqueous NaOH (5N, 5 ml), and hydrogen peroxide (30% aqueous, 9.7 ml). The reaction mixture was acidified to pH=2 with aqueous HCl (1 N) and extracted three times with CH2Cl2. The organic layers were combined, washed with brine, dried (Na2SO4), and stripped. The resulting alcohol 15-C was purified by silica gel chromatography eluting with a gradient 30-50% EtOAc/hexanes and isolated as a clear, colorless oil.
    • Step C:
  • A solution of alcohol 15-C (1.5 g, 7.1 mmol) in CH2Cl2 (7.5 ml), pyridine (1.5 ml) was cooled to 0° C. and treated with methanesulfonyl chloride (1.65 ml, 21.3 mmol), dropwise over 5 min. The reaction mixture was allowed to warm to room temperature, then stirred for 3 h. EtOAc (300 ml) was added and the organic phase was washed with aqueous HCl (1 N) three times, saturated aqueous sodium bicarbonate two times, and brine. The organic layer was dried (Na2SO4), and stripped to yield methyl 4-{2-[(methylsulfonyl)oxy]ethyl}bicyclo[2.2.2]octane-1-carboxylate 15-D as a white solid. 1H NMR (500 MHz, CDCl3): δ 1.52 (6H, m), 1.66 (2H, t, J=7.1 Hz), 1.84 (6H, m), 3.04 (3H, s), 3.69 (3H, s), 4.29 (2H, t, J=7.2 Hz) ppm.
    • Step D:
  • A solution of 15-D (0.25 g, 0.86 mmol), potassium trifluoromethanesulfinate (0.3 g, 1.72 mmol), and tetrabutylammonium iodide (0.15 g, 0.4 mmol) in DMF (5 ml) was heated at 140° C. for 5 h. under nitrogen atmosphere. The solution was then cooled to room temperature and diluted with EtOAc (100 ml) and washed with aqueous HCl (IN) two times and brine. The organic layer was dried (Na2SO4), stripped, and chromatographed on flash silica gel, eluting with a gradient 5-20% EtOAc/hexanes. The resulting trifluoromethylsulfone 15-E was isolated as a white solid. 1H NMR (500 MHz, CDCl3): δ 1.50 (6H, m), 1.78 (2H, m), 1.82 (6H, m), 3.17 (2H, m), 3.67 (3H, s) ppm.
    • Step E:
    • Methyl ester 15-E (0.035 g, 0.11 mmol) was converted to the methyl amide 15-F using the methods described in Example 10, steps C and D. The N-methyl-4-{2-[(trifluoromethyl)sulfonyl]ethyl}bicyclo[2.2.2]octane-1-carboxamide was isolated as a white solid; MS (ESI+)=328.2 (M+1).
    Step F:
  • Methyl amide 15-F (0.030 g, 0.092 mmol) was converted to triazole 15-G using the procedures outlined in Example 10, step E. 4-Methyl-3-[2-(trifluoromethyl)phenyl]-5-(4-{2-[(trifluoromethyl)sulfonyl]ethyl}bicyclo[2.2.2]oct-1-yl)-4H-1,2,4-triazole (15-G) was isolated as a white powder; MS (ESI+)=496.4 (M+1).
    • EXAMPLES 16-150
  • Following procedures similar to those described above, the following compounds of formula II were also prepared:
  • (II)
    Figure US20090181994A1-20090716-C00059
    Parent
    Ion
    Ex. # R3 R2 R1 m/z
    16
    Figure US20090181994A1-20090716-C00060
         		CH3
    Figure US20090181994A1-20090716-C00061
         		338
    17
    Figure US20090181994A1-20090716-C00062
         		CH3
    Figure US20090181994A1-20090716-C00063
         		406
    18
    Figure US20090181994A1-20090716-C00064
         		CH3
    Figure US20090181994A1-20090716-C00065
         		352
    19
    Figure US20090181994A1-20090716-C00066
         		CH3
    Figure US20090181994A1-20090716-C00067
         		372
    20
    Figure US20090181994A1-20090716-C00068
         		CH3
    Figure US20090181994A1-20090716-C00069
         		356
    21
    Figure US20090181994A1-20090716-C00070
         		CH3
    Figure US20090181994A1-20090716-C00071
         		368
    22
    Figure US20090181994A1-20090716-C00072
         		CH3
    Figure US20090181994A1-20090716-C00073
         		384
    23
    Figure US20090181994A1-20090716-C00074
         		CH3
    Figure US20090181994A1-20090716-C00075
         		383
    24
    Figure US20090181994A1-20090716-C00076
         		CH3
    Figure US20090181994A1-20090716-C00077
         		416
    25
    Figure US20090181994A1-20090716-C00078
         		CH3
    Figure US20090181994A1-20090716-C00079
         		422
    26
    Figure US20090181994A1-20090716-C00080
         		CH3
    Figure US20090181994A1-20090716-C00081
         		354
    27
    Figure US20090181994A1-20090716-C00082
         		CH3
    Figure US20090181994A1-20090716-C00083
         		382
    28
    Figure US20090181994A1-20090716-C00084
         		CH3
    Figure US20090181994A1-20090716-C00085
         		422
    29
    Figure US20090181994A1-20090716-C00086
         		CH3
    Figure US20090181994A1-20090716-C00087
         		368
    30
    Figure US20090181994A1-20090716-C00088
         		CH3
    Figure US20090181994A1-20090716-C00089
         		354
    31
    Figure US20090181994A1-20090716-C00090
         		CH3
    Figure US20090181994A1-20090716-C00091
         		496
    32
    Figure US20090181994A1-20090716-C00092
         		CH3
    Figure US20090181994A1-20090716-C00093
         		417
    33
    Figure US20090181994A1-20090716-C00094
         		CH3
    Figure US20090181994A1-20090716-C00095
         		372
    34
    Figure US20090181994A1-20090716-C00096
         		CH3
    Figure US20090181994A1-20090716-C00097
         		372
    35
    Figure US20090181994A1-20090716-C00098
         		CH3
    Figure US20090181994A1-20090716-C00099
         		352
    36
    Figure US20090181994A1-20090716-C00100
         		CH3
    Figure US20090181994A1-20090716-C00101
         		398
    37
    Figure US20090181994A1-20090716-C00102
         		CH3
    Figure US20090181994A1-20090716-C00103
         		382
    38
    Figure US20090181994A1-20090716-C00104
         		CH3
    Figure US20090181994A1-20090716-C00105
         		400
    39
    Figure US20090181994A1-20090716-C00106
         		CH3
    Figure US20090181994A1-20090716-C00107
         		368
    40
    Figure US20090181994A1-20090716-C00108
         		CH3
    Figure US20090181994A1-20090716-C00109
         		356
    41
    Figure US20090181994A1-20090716-C00110
         		CH3
    Figure US20090181994A1-20090716-C00111
         		366
    42
    Figure US20090181994A1-20090716-C00112
         		CH3
    Figure US20090181994A1-20090716-C00113
         		398
    43
    Figure US20090181994A1-20090716-C00114
         		CH3
    Figure US20090181994A1-20090716-C00115
         		374
    44
    Figure US20090181994A1-20090716-C00116
         		CH3
    Figure US20090181994A1-20090716-C00117
         		404
    45
    Figure US20090181994A1-20090716-C00118
         		CH3
    Figure US20090181994A1-20090716-C00119
         		374
    46
    Figure US20090181994A1-20090716-C00120
         		CH3
    Figure US20090181994A1-20090716-C00121
         		372
    47
    Figure US20090181994A1-20090716-C00122
         		CH3
    Figure US20090181994A1-20090716-C00123
         		372
    48
    Figure US20090181994A1-20090716-C00124
         		CH3
    Figure US20090181994A1-20090716-C00125
         		378
    49
    Figure US20090181994A1-20090716-C00126
         		CH3
    Figure US20090181994A1-20090716-C00127
         		402
    50
    Figure US20090181994A1-20090716-C00128
         		CH3
    Figure US20090181994A1-20090716-C00129
         		436
    51
    Figure US20090181994A1-20090716-C00130
         		CH3
    Figure US20090181994A1-20090716-C00131
         		370
    52
    Figure US20090181994A1-20090716-C00132
         		CH3
    Figure US20090181994A1-20090716-C00133
         		422
    53
    Figure US20090181994A1-20090716-C00134
         		CH3
    Figure US20090181994A1-20090716-C00135
         		366
    54
    Figure US20090181994A1-20090716-C00136
         		CH3
    Figure US20090181994A1-20090716-C00137
         		431
    55
    Figure US20090181994A1-20090716-C00138
         		CH3
    Figure US20090181994A1-20090716-C00139
         		382
    56
    Figure US20090181994A1-20090716-C00140
         		CH3
    Figure US20090181994A1-20090716-C00141
         		430
    57
    Figure US20090181994A1-20090716-C00142
         		CH3
    Figure US20090181994A1-20090716-C00143
         		414
    58
    Figure US20090181994A1-20090716-C00144
         		CH3
    Figure US20090181994A1-20090716-C00145
         		418
    59
    Figure US20090181994A1-20090716-C00146
         		CH3
    Figure US20090181994A1-20090716-C00147
         		474
    60
    Figure US20090181994A1-20090716-C00148
         		CH3
    Figure US20090181994A1-20090716-C00149
         		430
    61
    Figure US20090181994A1-20090716-C00150
         		CH3
    Figure US20090181994A1-20090716-C00151
         		353
    62
    Figure US20090181994A1-20090716-C00152
         		CH3
    Figure US20090181994A1-20090716-C00153
         		363
    63
    Figure US20090181994A1-20090716-C00154
         		CH3
    Figure US20090181994A1-20090716-C00155
         		366
    64
    Figure US20090181994A1-20090716-C00156
         		CH3
    Figure US20090181994A1-20090716-C00157
         		339
    65
    Figure US20090181994A1-20090716-C00158
         		CH3
    Figure US20090181994A1-20090716-C00159
         		339
    66
    Figure US20090181994A1-20090716-C00160
         		CH3
    Figure US20090181994A1-20090716-C00161
         		339
    67
    Figure US20090181994A1-20090716-C00162
         		CH3
    Figure US20090181994A1-20090716-C00163
         		355
    68
    Figure US20090181994A1-20090716-C00164
         		CH3
    Figure US20090181994A1-20090716-C00165
         		340
    69
    Figure US20090181994A1-20090716-C00166
         		CH3
    Figure US20090181994A1-20090716-C00167
         		388
    70
    Figure US20090181994A1-20090716-C00168
         		CH3
    Figure US20090181994A1-20090716-C00169
         		388
    71
    Figure US20090181994A1-20090716-C00170
         		CH3
    Figure US20090181994A1-20090716-C00171
         		378
    72
    Figure US20090181994A1-20090716-C00172
         		CH3
    Figure US20090181994A1-20090716-C00173
         		377
    73
    Figure US20090181994A1-20090716-C00174
         		CH3
    Figure US20090181994A1-20090716-C00175
         		389
    74
    Figure US20090181994A1-20090716-C00176
         		CH3
    Figure US20090181994A1-20090716-C00177
         		377
    75
    Figure US20090181994A1-20090716-C00178
         		CH3
    Figure US20090181994A1-20090716-C00179
         		380
    76
    Figure US20090181994A1-20090716-C00180
         		CH3
    Figure US20090181994A1-20090716-C00181
         		380
    77
    Figure US20090181994A1-20090716-C00182
         		CH3
    Figure US20090181994A1-20090716-C00183
         		382
    78
    Figure US20090181994A1-20090716-C00184
         		CH3
    Figure US20090181994A1-20090716-C00185
         		378
    79
    Figure US20090181994A1-20090716-C00186
         		CH2CH3
    Figure US20090181994A1-20090716-C00187
         		382
    80
    Figure US20090181994A1-20090716-C00188
         		CH2CH3
    Figure US20090181994A1-20090716-C00189
         		382
    81
    Figure US20090181994A1-20090716-C00190
         		CH2CH3
    Figure US20090181994A1-20090716-C00191
         		352
    82
    Figure US20090181994A1-20090716-C00192
         		CH2CH3
    Figure US20090181994A1-20090716-C00193
         		368
    83
    Figure US20090181994A1-20090716-C00194
         		CH2CH3
    Figure US20090181994A1-20090716-C00195
         		380
    84
    Figure US20090181994A1-20090716-C00196
         		CH2CH3
    Figure US20090181994A1-20090716-C00197
         		366
    85
    Figure US20090181994A1-20090716-C00198
    Figure US20090181994A1-20090716-C00199
    Figure US20090181994A1-20090716-C00200
         		364
    86
    Figure US20090181994A1-20090716-C00201
         		CH3
    Figure US20090181994A1-20090716-C00202
         		373
    87
    Figure US20090181994A1-20090716-C00203
         		CH3
    Figure US20090181994A1-20090716-C00204
         		389
    88
    Figure US20090181994A1-20090716-C00205
    Figure US20090181994A1-20090716-C00206
    Figure US20090181994A1-20090716-C00207
         		365
    89
    Figure US20090181994A1-20090716-C00208
         		CH3
    Figure US20090181994A1-20090716-C00209
         		340
    90
    Figure US20090181994A1-20090716-C00210
         		CH3
    Figure US20090181994A1-20090716-C00211
         		378
    91
    Figure US20090181994A1-20090716-C00212
         		CH3
    Figure US20090181994A1-20090716-C00213
         		345
    92
    Figure US20090181994A1-20090716-C00214
         		CH3
    Figure US20090181994A1-20090716-C00215
         		340
    93
    Figure US20090181994A1-20090716-C00216
         		CH3
    Figure US20090181994A1-20090716-C00217
         		326
    94
    Figure US20090181994A1-20090716-C00218
         		CH3
    Figure US20090181994A1-20090716-C00219
         		354
    95
    Figure US20090181994A1-20090716-C00220
         		CH3
    Figure US20090181994A1-20090716-C00221
         		361
    96
    Figure US20090181994A1-20090716-C00222
         		CH3
    Figure US20090181994A1-20090716-C00223
         		356
    97
    Figure US20090181994A1-20090716-C00224
         		CH3
    Figure US20090181994A1-20090716-C00225
         		340
    98
    Figure US20090181994A1-20090716-C00226
         		CH3
    Figure US20090181994A1-20090716-C00227
         		343
    99
    Figure US20090181994A1-20090716-C00228
         		CH3
    Figure US20090181994A1-20090716-C00229
         		338
    100
    Figure US20090181994A1-20090716-C00230
         		CH3
    Figure US20090181994A1-20090716-C00231
         		364
    101
    Figure US20090181994A1-20090716-C00232
         		CH3
    Figure US20090181994A1-20090716-C00233
         		326
    102
    Figure US20090181994A1-20090716-C00234
         		CH3
    Figure US20090181994A1-20090716-C00235
         		312
    103
    Figure US20090181994A1-20090716-C00236
         		CH3
    Figure US20090181994A1-20090716-C00237
         		331
    104
    Figure US20090181994A1-20090716-C00238
         		CH3
    Figure US20090181994A1-20090716-C00239
         		342
    105
    Figure US20090181994A1-20090716-C00240
         		CH3
    Figure US20090181994A1-20090716-C00241
         		326
    106
    Figure US20090181994A1-20090716-C00242
         		CH3
    Figure US20090181994A1-20090716-C00243
         		340
    107
    Figure US20090181994A1-20090716-C00244
         		CH3
    Figure US20090181994A1-20090716-C00245
         		361
    108
    Figure US20090181994A1-20090716-C00246
         		CH3
    Figure US20090181994A1-20090716-C00247
         		356
    109
    Figure US20090181994A1-20090716-C00248
         		CH3
    Figure US20090181994A1-20090716-C00249
         		365
    110
    Figure US20090181994A1-20090716-C00250
         		CH3
    Figure US20090181994A1-20090716-C00251
         		382
    111
    Figure US20090181994A1-20090716-C00252
         		CH3
    Figure US20090181994A1-20090716-C00253
         		358
    112
    Figure US20090181994A1-20090716-C00254
         		CH3
    Figure US20090181994A1-20090716-C00255
         		379
    113
    Figure US20090181994A1-20090716-C00256
         		CH3
    Figure US20090181994A1-20090716-C00257
         		407
    114
    Figure US20090181994A1-20090716-C00258
         		CH3
    Figure US20090181994A1-20090716-C00259
         		438
    115 CH3 CH3
    Figure US20090181994A1-20090716-C00260
         		282
    116
    Figure US20090181994A1-20090716-C00261
         		CH3
    Figure US20090181994A1-20090716-C00262
         		348
    117 H CH3
    Figure US20090181994A1-20090716-C00263
         		284
    118 H CH3
    Figure US20090181994A1-20090716-C00264
         		298
    119 H CH3
    Figure US20090181994A1-20090716-C00265
         		302
    120 H CH3
    Figure US20090181994A1-20090716-C00266
         		298
    121 H CH3
    Figure US20090181994A1-20090716-C00267
         		336
    122
    Figure US20090181994A1-20090716-C00268
         		CH3
    Figure US20090181994A1-20090716-C00269
         		344
    123
    Figure US20090181994A1-20090716-C00270
         		CH3
    Figure US20090181994A1-20090716-C00271
         		374
    124
    Figure US20090181994A1-20090716-C00272
         		CH3
    Figure US20090181994A1-20090716-C00273
         		358
    125
    Figure US20090181994A1-20090716-C00274
         		CH3
    Figure US20090181994A1-20090716-C00275
         		360
    126
    Figure US20090181994A1-20090716-C00276
         		CH3
    Figure US20090181994A1-20090716-C00277
         		471
    127
    Figure US20090181994A1-20090716-C00278
         		CH3
    Figure US20090181994A1-20090716-C00279
         		456
    128
    Figure US20090181994A1-20090716-C00280
         		CH3
    Figure US20090181994A1-20090716-C00281
         		326
    129 CbzNH— CH3
    Figure US20090181994A1-20090716-C00282
         		428
    130 NH2 CH3
    Figure US20090181994A1-20090716-C00283
         		313
    131
    Figure US20090181994A1-20090716-C00284
         		CH3
    Figure US20090181994A1-20090716-C00285
         		450
    132
    Figure US20090181994A1-20090716-C00286
         		CH3
    Figure US20090181994A1-20090716-C00287
         		421
    133
    Figure US20090181994A1-20090716-C00288
         		CH3
    Figure US20090181994A1-20090716-C00289
         		422
    134
    Figure US20090181994A1-20090716-C00290
         		CH3
    Figure US20090181994A1-20090716-C00291
         		402
    135
    Figure US20090181994A1-20090716-C00292
         		CH3
    Figure US20090181994A1-20090716-C00293
         		456
    136
    Figure US20090181994A1-20090716-C00294
         		CH3
    Figure US20090181994A1-20090716-C00295
         		470
    137
    Figure US20090181994A1-20090716-C00296
         		CH3
    Figure US20090181994A1-20090716-C00297
         		442
    138
    Figure US20090181994A1-20090716-C00298
         		CH3
    Figure US20090181994A1-20090716-C00299
         		440
    139
    Figure US20090181994A1-20090716-C00300
         		CH3
    Figure US20090181994A1-20090716-C00301
         		470
    140
    Figure US20090181994A1-20090716-C00302
         		CH3
    Figure US20090181994A1-20090716-C00303
         		484
    141
    Figure US20090181994A1-20090716-C00304
         		CH3
    Figure US20090181994A1-20090716-C00305
         		490
    142
    Figure US20090181994A1-20090716-C00306
         		CH3
    Figure US20090181994A1-20090716-C00307
         		508
    143
    Figure US20090181994A1-20090716-C00308
         		CH3
    Figure US20090181994A1-20090716-C00309
         		420
  • Furthermore following procedure similar to those described above, the following compounds of formula III were also prepared:
  • (III)
    Figure US20090181994A1-20090716-C00310
    Parent
    Ion
    Ex. # R5 R1 m/z
    144 Cl
    Figure US20090181994A1-20090716-C00311
         		477
    145 Cl
    Figure US20090181994A1-20090716-C00312
         		515
    146 Cl
    Figure US20090181994A1-20090716-C00313
         		480
    147 Cl
    Figure US20090181994A1-20090716-C00314
         		511
    148 Cl
    Figure US20090181994A1-20090716-C00315
         		497
    149 F
    Figure US20090181994A1-20090716-C00316
         		476
    150 F
    Figure US20090181994A1-20090716-C00317
         		567
    • Example of a Pharmaceutical Formulation
  • As a specific embodiment of an oral composition of a compound of the present invention, 50 mg of any of Examples 1-15 is formulated with sufficient finely divided lactose to provide a total amount of 580 to 590 mg to fill a size O hard gelatin capsule.
  • While the invention has been described and illustrated in reference to specific embodiments thereof, those skilled in the art will appreciate that various changes, modifications, and substitutions can be made therein without departing from the spirit and scope of the invention. For example, effective dosages other than the preferred doses as set forth hereinabove may be applicable as a consequence of variations in the responsiveness of the human being treated for a particular condition. Likewise, the pharmacologic response observed may vary according to and depending upon the particular active compound selected or whether there are present pharmaceutical carriers, as well as the type of formulation and mode of administration employed, and such expected variations or differences in the results are contemplated in accordance with the objects and practices of the present invention. It is intended therefore that the invention be limited only by the scope of the claims which follow and that such claims be interpreted as broadly as is reasonable.

Claims (16)

1. A compound which is
Figure US20090181994A1-20090716-C00318
or a pharmaceutically acceptable salt thereof.
2. A method of treating cognitive impairment in a mammalian patient comprising administering to the patient an effective amount of a compound selected from the group consisting of structural formula I:
Figure US20090181994A1-20090716-C00319
or a pharmaceutically acceptable salt thereof; wherein
each p is independently 0, 1, or 2;
each n is independently 0, 1, or 2;
X is selected from the group consisting of a single bond, O, S(O)p, NR6,
Figure US20090181994A1-20090716-C00320
R1 is selected from the group consisting of
arylcarbonyl,
(CH2)n-aryl, and
(CH2)n-heteroaryl;
in which aryl and heteroaryl are unsubstituted or substituted with one to three substituents independently selected from R5;
R2 is selected from the group consisting of
hydrogen,
C1-8 alkyl,
C2-6 alkenyl, and
(CH2)n—C3-6 cycloalkyl;
in which alkyl, alkenyl, and cycloalkyl are unsubstituted or substituted with one to three substituents independently selected from R8 and oxo;
each R4 is independently selected from the group consisting of
hydrogen,
halogen,
hydroxy,
oxo,
C1-3 alkyl, and
C1-3 alkoxy;
R3 is selected from the group consisting of
hydrogen,
C1-10 alkyl
C2-10 alkenyl,
(CH2)n—C3-6 cycloalkyl,
(CH2)n-aryl, and
(CH2)n-heteroaryl;
(CH2)n-heterocyclyl;
in which aryl, heteroaryl and heterocyclyl are unsubstituted or substituted with one to three substituents independently selected from R5; and alkyl, alkenyl, and cycloalkyl are unsubstituted or substituted with one to five groups independently selected from R8 and oxo;
R5 and R8 are independently selected from the group consisting of
hydrogen,
formyl,
C1-6 alkyl,
(CH2)n-aryl,
(CH2)n-heteroaryl,
(CH2)n-heterocyclyl,
(CH2)nC3-7 cycloalkyl,
halogen,
OR7,
(CH2)nN(R7)2,
cyano,
(CH2)nCO2R7,
NO2,
(CH2)nNR7SO2R6,
(CH2)nSO2N(R7)2,
(CH2)nS(O)pR6,
(CH2)nSO20R7,
(CH2)nNR7C(O)N(R7)2,
(CH2)nC(O)N(R7)2,
(CH2)nNR6C(O)R6,
(CH2)nNR6CO2R7,
O(CH2)nC(O)N(R7)2,
CF3,
CH2CF3,
OCF3,
OCHCF2, and
OCH2CF3;
wherein aryl, heteroaryl, cycloalkyl, and heterocyclyl are unsubstituted or substituted with one to three substituents independently selected from halogen, hydroxy, C1-4 alkyl, trifluoromethyl, trifluoromethoxy, and C1-4 alkoxy; and wherein any methylene (CH2) carbon atom in R5 and R8 is unsubstituted or substituted with one to two groups independently selected from halogen, hydroxy, and C1-4 alkyl; or two substituents when on the same methylene (CH2) carbon atom are taken together with the carbon atom to which they are attached to form a cyclopropyl group;
each R6 is independently selected from the group consisting of
C1-8 alkyl,
(CH2)n-aryl,
(CH2)n-heteroaryl, and
(CH2)nC3-7 cycloalkyl;
wherein alkyl and cycloalkyl are unsubstituted or substituted with one to five substituents independently selected from halogen, oxo, C1-4 alkoxy, C1-4 alkylthio, hydroxy, amino; and aryl and heteroaryl are unsubstituted or substituted with one to three substituents independently selected from cyano, halogen, hydroxy, amino, carboxy, trifluoromethyl, trifluoromethoxy, C1-4 alkyl, and C1-4 alkoxy;
or two R6 groups together with the atom to which they are attached form a 5- to 8-membered mono- or bicyclic ring system optionally containing an additional heteroatom selected from O, S, and NC1-4 alkyl;
and
each R7 is hydrogen or R6;
structural formula II, or a pharmaceutically acceptable salt thereof
(II)
Figure US20090181994A1-20090716-C00321
 wherein R3 R2 R1
Figure US20090181994A1-20090716-C00322
 CH3
Figure US20090181994A1-20090716-C00323
Figure US20090181994A1-20090716-C00324
 CH3
Figure US20090181994A1-20090716-C00325
Figure US20090181994A1-20090716-C00326
 CH3
Figure US20090181994A1-20090716-C00327
Figure US20090181994A1-20090716-C00328
 CH3
Figure US20090181994A1-20090716-C00329
Figure US20090181994A1-20090716-C00330
 CH3
Figure US20090181994A1-20090716-C00331
Figure US20090181994A1-20090716-C00332
 CH3
Figure US20090181994A1-20090716-C00333
Figure US20090181994A1-20090716-C00334
 CH3
Figure US20090181994A1-20090716-C00335
Figure US20090181994A1-20090716-C00336
 CH3
Figure US20090181994A1-20090716-C00337
Figure US20090181994A1-20090716-C00338
 CH3
Figure US20090181994A1-20090716-C00339
Figure US20090181994A1-20090716-C00340
 CH3
Figure US20090181994A1-20090716-C00341
Figure US20090181994A1-20090716-C00342
 CH3
Figure US20090181994A1-20090716-C00343
Figure US20090181994A1-20090716-C00344
 CH3
Figure US20090181994A1-20090716-C00345
Figure US20090181994A1-20090716-C00346
 CH3
Figure US20090181994A1-20090716-C00347
Figure US20090181994A1-20090716-C00348
 CH3
Figure US20090181994A1-20090716-C00349
Figure US20090181994A1-20090716-C00350
 CH3
Figure US20090181994A1-20090716-C00351
Figure US20090181994A1-20090716-C00352
 CH3
Figure US20090181994A1-20090716-C00353
Figure US20090181994A1-20090716-C00354
 CH3
Figure US20090181994A1-20090716-C00355
Figure US20090181994A1-20090716-C00356
 CH3
Figure US20090181994A1-20090716-C00357
Figure US20090181994A1-20090716-C00358
 CH3
Figure US20090181994A1-20090716-C00359
Figure US20090181994A1-20090716-C00360
 CH3
Figure US20090181994A1-20090716-C00361
Figure US20090181994A1-20090716-C00362
 CH3
Figure US20090181994A1-20090716-C00363
Figure US20090181994A1-20090716-C00364
 CH3
Figure US20090181994A1-20090716-C00365
Figure US20090181994A1-20090716-C00366
 CH3
Figure US20090181994A1-20090716-C00367
Figure US20090181994A1-20090716-C00368
 CH3
Figure US20090181994A1-20090716-C00369
Figure US20090181994A1-20090716-C00370
 CH3
Figure US20090181994A1-20090716-C00371
Figure US20090181994A1-20090716-C00372
 CH3
Figure US20090181994A1-20090716-C00373
Figure US20090181994A1-20090716-C00374
 CH3
Figure US20090181994A1-20090716-C00375
Figure US20090181994A1-20090716-C00376
 CH3
Figure US20090181994A1-20090716-C00377
Figure US20090181994A1-20090716-C00378
 CH3
Figure US20090181994A1-20090716-C00379
Figure US20090181994A1-20090716-C00380
 CH3
Figure US20090181994A1-20090716-C00381
Figure US20090181994A1-20090716-C00382
 CH3
Figure US20090181994A1-20090716-C00383
Figure US20090181994A1-20090716-C00384
 CH3
Figure US20090181994A1-20090716-C00385
Figure US20090181994A1-20090716-C00386
 CH3
Figure US20090181994A1-20090716-C00387
Figure US20090181994A1-20090716-C00388
 CH3
Figure US20090181994A1-20090716-C00389
Figure US20090181994A1-20090716-C00390
 CH3
Figure US20090181994A1-20090716-C00391
Figure US20090181994A1-20090716-C00392
 CH3
Figure US20090181994A1-20090716-C00393
Figure US20090181994A1-20090716-C00394
 CH3
Figure US20090181994A1-20090716-C00395
Figure US20090181994A1-20090716-C00396
 CH3
Figure US20090181994A1-20090716-C00397
Figure US20090181994A1-20090716-C00398
 CH3
Figure US20090181994A1-20090716-C00399
Figure US20090181994A1-20090716-C00400
 CH3
Figure US20090181994A1-20090716-C00401
Figure US20090181994A1-20090716-C00402
 CH3
Figure US20090181994A1-20090716-C00403
Figure US20090181994A1-20090716-C00404
 CH3
Figure US20090181994A1-20090716-C00405
Figure US20090181994A1-20090716-C00406
 CH3
Figure US20090181994A1-20090716-C00407
Figure US20090181994A1-20090716-C00408
 CH3
Figure US20090181994A1-20090716-C00409
Figure US20090181994A1-20090716-C00410
 CH3
Figure US20090181994A1-20090716-C00411
Figure US20090181994A1-20090716-C00412
 CH3
Figure US20090181994A1-20090716-C00413
Figure US20090181994A1-20090716-C00414
 CH3
Figure US20090181994A1-20090716-C00415
Figure US20090181994A1-20090716-C00416
 CH3
Figure US20090181994A1-20090716-C00417
Figure US20090181994A1-20090716-C00418
 CH3
Figure US20090181994A1-20090716-C00419
Figure US20090181994A1-20090716-C00420
 CH3
Figure US20090181994A1-20090716-C00421
Figure US20090181994A1-20090716-C00422
 CH3
Figure US20090181994A1-20090716-C00423
Figure US20090181994A1-20090716-C00424
 CH3
Figure US20090181994A1-20090716-C00425
Figure US20090181994A1-20090716-C00426
 CH3
Figure US20090181994A1-20090716-C00427
Figure US20090181994A1-20090716-C00428
 CH3
Figure US20090181994A1-20090716-C00429
Figure US20090181994A1-20090716-C00430
 CH3
Figure US20090181994A1-20090716-C00431
Figure US20090181994A1-20090716-C00432
 CH3
Figure US20090181994A1-20090716-C00433
Figure US20090181994A1-20090716-C00434
 CH3
Figure US20090181994A1-20090716-C00435
Figure US20090181994A1-20090716-C00436
 CH3
Figure US20090181994A1-20090716-C00437
Figure US20090181994A1-20090716-C00438
 CH3
Figure US20090181994A1-20090716-C00439
Figure US20090181994A1-20090716-C00440
 CH3
Figure US20090181994A1-20090716-C00441
Figure US20090181994A1-20090716-C00442
 CH3
Figure US20090181994A1-20090716-C00443
Figure US20090181994A1-20090716-C00444
 CH3
Figure US20090181994A1-20090716-C00445
Figure US20090181994A1-20090716-C00446
 CH3
Figure US20090181994A1-20090716-C00447
Figure US20090181994A1-20090716-C00448
 CH3
Figure US20090181994A1-20090716-C00449
Figure US20090181994A1-20090716-C00450
 CH3
Figure US20090181994A1-20090716-C00451
Figure US20090181994A1-20090716-C00452
 CH3
Figure US20090181994A1-20090716-C00453
Figure US20090181994A1-20090716-C00454
 CH2CH3
Figure US20090181994A1-20090716-C00455
Figure US20090181994A1-20090716-C00456
 CH2CH3
Figure US20090181994A1-20090716-C00457
Figure US20090181994A1-20090716-C00458
 CH2CH3
Figure US20090181994A1-20090716-C00459
Figure US20090181994A1-20090716-C00460
 CH2CH3
Figure US20090181994A1-20090716-C00461
Figure US20090181994A1-20090716-C00462
 CH2CH3
Figure US20090181994A1-20090716-C00463
Figure US20090181994A1-20090716-C00464
 CH2CH3
Figure US20090181994A1-20090716-C00465
Figure US20090181994A1-20090716-C00466
Figure US20090181994A1-20090716-C00467
Figure US20090181994A1-20090716-C00468
Figure US20090181994A1-20090716-C00469
 CH3
Figure US20090181994A1-20090716-C00470
Figure US20090181994A1-20090716-C00471
 CH3
Figure US20090181994A1-20090716-C00472
Figure US20090181994A1-20090716-C00473
Figure US20090181994A1-20090716-C00474
Figure US20090181994A1-20090716-C00475
Figure US20090181994A1-20090716-C00476
 CH3
Figure US20090181994A1-20090716-C00477
Figure US20090181994A1-20090716-C00478
 CH3
Figure US20090181994A1-20090716-C00479
Figure US20090181994A1-20090716-C00480
 CH3
Figure US20090181994A1-20090716-C00481
Figure US20090181994A1-20090716-C00482
 CH3
Figure US20090181994A1-20090716-C00483
Figure US20090181994A1-20090716-C00484
 CH3
Figure US20090181994A1-20090716-C00485
Figure US20090181994A1-20090716-C00486
 CH3
Figure US20090181994A1-20090716-C00487
Figure US20090181994A1-20090716-C00488
 CH3
Figure US20090181994A1-20090716-C00489
Figure US20090181994A1-20090716-C00490
 CH3
Figure US20090181994A1-20090716-C00491
Figure US20090181994A1-20090716-C00492
 CH3
Figure US20090181994A1-20090716-C00493
Figure US20090181994A1-20090716-C00494
 CH3
Figure US20090181994A1-20090716-C00495
Figure US20090181994A1-20090716-C00496
 CH3
Figure US20090181994A1-20090716-C00497
Figure US20090181994A1-20090716-C00498
 CH3
Figure US20090181994A1-20090716-C00499
Figure US20090181994A1-20090716-C00500
 CH3
Figure US20090181994A1-20090716-C00501
Figure US20090181994A1-20090716-C00502
 CH3
Figure US20090181994A1-20090716-C00503
Figure US20090181994A1-20090716-C00504
 CH3
Figure US20090181994A1-20090716-C00505
Figure US20090181994A1-20090716-C00506
 CH3
Figure US20090181994A1-20090716-C00507
Figure US20090181994A1-20090716-C00508
 CH3
Figure US20090181994A1-20090716-C00509
Figure US20090181994A1-20090716-C00510
 CH3
Figure US20090181994A1-20090716-C00511
Figure US20090181994A1-20090716-C00512
 CH3
Figure US20090181994A1-20090716-C00513
Figure US20090181994A1-20090716-C00514
 CH3
Figure US20090181994A1-20090716-C00515
Figure US20090181994A1-20090716-C00516
 CH3
Figure US20090181994A1-20090716-C00517
Figure US20090181994A1-20090716-C00518
 CH3
Figure US20090181994A1-20090716-C00519
Figure US20090181994A1-20090716-C00520
 CH3
Figure US20090181994A1-20090716-C00521
Figure US20090181994A1-20090716-C00522
 CH3
Figure US20090181994A1-20090716-C00523
Figure US20090181994A1-20090716-C00524
 CH3
Figure US20090181994A1-20090716-C00525
Figure US20090181994A1-20090716-C00526
 CH3
Figure US20090181994A1-20090716-C00527
Figure US20090181994A1-20090716-C00528
 CH3
Figure US20090181994A1-20090716-C00529
Figure US20090181994A1-20090716-C00530
 CH3
Figure US20090181994A1-20090716-C00531
Figure US20090181994A1-20090716-C00532
 CH3
Figure US20090181994A1-20090716-C00533
Figure US20090181994A1-20090716-C00534
 CH3
Figure US20090181994A1-20090716-C00535
 CH3 CH3
Figure US20090181994A1-20090716-C00536
Figure US20090181994A1-20090716-C00537
 CH3
Figure US20090181994A1-20090716-C00538
 H CH3
Figure US20090181994A1-20090716-C00539
 H CH3
Figure US20090181994A1-20090716-C00540
 H CH3
Figure US20090181994A1-20090716-C00541
 H CH3
Figure US20090181994A1-20090716-C00542
 H CH3
Figure US20090181994A1-20090716-C00543
Figure US20090181994A1-20090716-C00544
 CH3
Figure US20090181994A1-20090716-C00545
Figure US20090181994A1-20090716-C00546
 CH3
Figure US20090181994A1-20090716-C00547
Figure US20090181994A1-20090716-C00548
 CH3
Figure US20090181994A1-20090716-C00549
Figure US20090181994A1-20090716-C00550
 CH3
Figure US20090181994A1-20090716-C00551
Figure US20090181994A1-20090716-C00552
 CH3
Figure US20090181994A1-20090716-C00553
Figure US20090181994A1-20090716-C00554
 CH3
Figure US20090181994A1-20090716-C00555
Figure US20090181994A1-20090716-C00556
 CH3
Figure US20090181994A1-20090716-C00557
Figure US20090181994A1-20090716-C00558
 CH3
Figure US20090181994A1-20090716-C00559
Figure US20090181994A1-20090716-C00560
 CH3
Figure US20090181994A1-20090716-C00561
 CbzNH— CH3
Figure US20090181994A1-20090716-C00562
 NH2 CH3
Figure US20090181994A1-20090716-C00563
Figure US20090181994A1-20090716-C00564
 CH3
Figure US20090181994A1-20090716-C00565
Figure US20090181994A1-20090716-C00566
 CH3
Figure US20090181994A1-20090716-C00567
Figure US20090181994A1-20090716-C00568
 CH3
Figure US20090181994A1-20090716-C00569
Figure US20090181994A1-20090716-C00570
 CH3
Figure US20090181994A1-20090716-C00571
Figure US20090181994A1-20090716-C00572
 CH3
Figure US20090181994A1-20090716-C00573
Figure US20090181994A1-20090716-C00574
 CH3
Figure US20090181994A1-20090716-C00575
Figure US20090181994A1-20090716-C00576
 CH3
Figure US20090181994A1-20090716-C00577
Figure US20090181994A1-20090716-C00578
 CH3
Figure US20090181994A1-20090716-C00579
Figure US20090181994A1-20090716-C00580
 CH3
Figure US20090181994A1-20090716-C00581
Figure US20090181994A1-20090716-C00582
 CH3
Figure US20090181994A1-20090716-C00583
Figure US20090181994A1-20090716-C00584
 CH3
Figure US20090181994A1-20090716-C00585
Figure US20090181994A1-20090716-C00586
 CH3
Figure US20090181994A1-20090716-C00587
Figure US20090181994A1-20090716-C00588
 CH3
Figure US20090181994A1-20090716-C00589
Figure US20090181994A1-20090716-C00590
 CH3
Figure US20090181994A1-20090716-C00591
Figure US20090181994A1-20090716-C00592
 CH3
Figure US20090181994A1-20090716-C00593
Figure US20090181994A1-20090716-C00594
 CH3
Figure US20090181994A1-20090716-C00595
Figure US20090181994A1-20090716-C00596
 CH3
Figure US20090181994A1-20090716-C00597
Figure US20090181994A1-20090716-C00598
 CH3
Figure US20090181994A1-20090716-C00599
and structural formula III, or a pharmaceutically acceptable salt thereof
(III)
Figure US20090181994A1-20090716-C00600
 wherein R5′ R1 Cl
Figure US20090181994A1-20090716-C00601
 Cl
Figure US20090181994A1-20090716-C00602
 Cl
Figure US20090181994A1-20090716-C00603
 Cl
Figure US20090181994A1-20090716-C00604
 Cl
Figure US20090181994A1-20090716-C00605
 F
Figure US20090181994A1-20090716-C00606
 F
Figure US20090181994A1-20090716-C00607
 F
Figure US20090181994A1-20090716-C00608
or a pharmaceutically acceptable salt thereof.
3. A method in accordance with claim 2, wherein the compound administered is selected from the group consisting of:
Figure US20090181994A1-20090716-C00609
Figure US20090181994A1-20090716-C00610
or a pharmaceutically acceptable salt thereof.
4. A method in accordance with claim 2, wherein the compound administered is selected from the group consisting of
Figure US20090181994A1-20090716-C00611
or a pharmaceutically acceptable salt thereof.
5. A method of delaying the onset of cognitive impairment in a mammalian patient in need thereof comprising administering to the patient an effective amount of a compound selected from the group consisting of structural formula I:
Figure US20090181994A1-20090716-C00612
or a pharmaceutically acceptable salt thereof; wherein
each p is independently 0, 1, or 2;
each n is independently 0, 1, or 2;
X is selected from the group consisting of a single bond, O, S(O)p, NR6,
Figure US20090181994A1-20090716-C00613
R1 is selected from the group consisting of
arylcarbonyl,
(CH2)n-aryl, and
(CH2)n-heteroaryl;
in which aryl and heteroaryl are unsubstituted or substituted with one to three substituents independently selected from R5;
R2 is selected from the group consisting of
hydrogen,
C1-8 alkyl,
C2-6 alkenyl, and
(CH2)n—C3-6 cycloalkyl;
in which alkyl, alkenyl, and cycloalkyl are unsubstituted or substituted with one to three substituents independently selected from R8 and oxo;
each R4 is independently selected from the group consisting of
hydrogen,
halogen,
hydroxy,
oxo,
C1-3 alkyl, and
C1-3 alkoxy;
R3 is selected from the group consisting of
hydrogen,
C1-10 alkyl
C2-10 alkenyl,
(CH2)n—C3-6 cycloalkyl,
(CH2)n-aryl, and
(CH2)n-heteroaryl;
(CH2)n-heterocyclyl;
in which aryl, heteroaryl and heterocyclyl are unsubstituted or substituted with one to three substituents independently selected from R5; and alkyl, alkenyl, and cycloalkyl are unsubstituted or substituted with one to five groups independently selected from R8 and oxo;
R5 and R8 are independently selected from the group consisting of
hydrogen,
formyl,
C1-6 alkyl,
(CH2)n-aryl,
(CH2)n-heteroaryl,
(CH2)n-heterocyclyl,
(CH2)nC3-7 cycloalkyl,
halogen,
OR7,
(CH2)nN(R7)2,
cyano,
(CH2)nCO2R7,
NO2,
(CH2)nNR7SO2R6,
(CH2)nSO2N(R7)2,
(CH2)nS(O)pR6,
(CH2)nSO20R7,
(CH2)nNR7C(O)N(R7)2,
(CH2)nC(O)N(R7)2,
(CH2)nNR6C(O)R6,
(CH2)nNR6CO2R7, O(CH2)nC(O)N(R7)2,
CF3,
CH2CF3,
OCF3,
OCHCF2, and
OCH2CF3;
wherein aryl, heteroaryl, cycloalkyl, and heterocyclyl are unsubstituted or substituted with one to three substituents independently selected from halogen, hydroxy, C1-4 alkyl, trifluoromethyl, trifluoromethoxy, and C1-4 alkoxy; and wherein any methylene (CH2) carbon atom in R5 and R8 is unsubstituted or substituted with one to two groups independently selected from halogen, hydroxy, and C1-4 alkyl; or two substituents when on the same methylene (CH2) carbon atom are taken together with the carbon atom to which they are attached to form a cyclopropyl group;
each R6 is independently selected from the group consisting of
C1-8 alkyl,
(CH2)n-aryl,
(CH2)n-heteroaryl, and
(CH2)nC3-7 cycloalkyl;
wherein alkyl and cycloalkyl are unsubstituted or substituted with one to five substituents independently selected from halogen, oxo, C1-4 alkoxy, C1-4 alkylthio, hydroxy, amino; and aryl and heteroaryl are unsubstituted or substituted with one to three substituents independently selected from cyano, halogen, hydroxy, amino, carboxy, trifluoromethyl, trifluoromethoxy, C1-4 alkyl, and C1-4 alkoxy;
or two R6 groups together with the atom to which they are attached form a 5- to 8-membered mono- or bicyclic ring system optionally containing an additional heteroatom selected from O, S, and NC1-4 alkyl;
and
each R7 is hydrogen or R6;
structural formula II, or a pharmaceutically acceptable salt thereof
(II)
Figure US20090181994A1-20090716-C00614
 wherein R3 R2 R1
Figure US20090181994A1-20090716-C00615
 CH3
Figure US20090181994A1-20090716-C00616
Figure US20090181994A1-20090716-C00617
 CH3
Figure US20090181994A1-20090716-C00618
Figure US20090181994A1-20090716-C00619
 CH3
Figure US20090181994A1-20090716-C00620
Figure US20090181994A1-20090716-C00621
 CH3
Figure US20090181994A1-20090716-C00622
Figure US20090181994A1-20090716-C00623
 CH3
Figure US20090181994A1-20090716-C00624
Figure US20090181994A1-20090716-C00625
 CH3
Figure US20090181994A1-20090716-C00626
Figure US20090181994A1-20090716-C00627
 CH3
Figure US20090181994A1-20090716-C00628
Figure US20090181994A1-20090716-C00629
 CH3
Figure US20090181994A1-20090716-C00630
Figure US20090181994A1-20090716-C00631
 CH3
Figure US20090181994A1-20090716-C00632
Figure US20090181994A1-20090716-C00633
 CH3
Figure US20090181994A1-20090716-C00634
Figure US20090181994A1-20090716-C00635
 CH3
Figure US20090181994A1-20090716-C00636
Figure US20090181994A1-20090716-C00637
 CH3
Figure US20090181994A1-20090716-C00638
Figure US20090181994A1-20090716-C00639
 CH3
Figure US20090181994A1-20090716-C00640
Figure US20090181994A1-20090716-C00641
 CH3
Figure US20090181994A1-20090716-C00642
Figure US20090181994A1-20090716-C00643
 CH3
Figure US20090181994A1-20090716-C00644
Figure US20090181994A1-20090716-C00645
 CH3
Figure US20090181994A1-20090716-C00646
Figure US20090181994A1-20090716-C00647
 CH3
Figure US20090181994A1-20090716-C00648
Figure US20090181994A1-20090716-C00649
 CH3
Figure US20090181994A1-20090716-C00650
Figure US20090181994A1-20090716-C00651
 CH3
Figure US20090181994A1-20090716-C00652
Figure US20090181994A1-20090716-C00653
 CH3
Figure US20090181994A1-20090716-C00654
Figure US20090181994A1-20090716-C00655
 CH3
Figure US20090181994A1-20090716-C00656
Figure US20090181994A1-20090716-C00657
 CH3
Figure US20090181994A1-20090716-C00658
Figure US20090181994A1-20090716-C00659
 CH3
Figure US20090181994A1-20090716-C00660
Figure US20090181994A1-20090716-C00661
 CH3
Figure US20090181994A1-20090716-C00662
Figure US20090181994A1-20090716-C00663
 CH3
Figure US20090181994A1-20090716-C00664
Figure US20090181994A1-20090716-C00665
 CH3
Figure US20090181994A1-20090716-C00666
Figure US20090181994A1-20090716-C00667
 CH3
Figure US20090181994A1-20090716-C00668
Figure US20090181994A1-20090716-C00669
 CH3
Figure US20090181994A1-20090716-C00670
Figure US20090181994A1-20090716-C00671
 CH3
Figure US20090181994A1-20090716-C00672
Figure US20090181994A1-20090716-C00673
 CH3
Figure US20090181994A1-20090716-C00674
Figure US20090181994A1-20090716-C00675
 CH3
Figure US20090181994A1-20090716-C00676
Figure US20090181994A1-20090716-C00677
 CH3
Figure US20090181994A1-20090716-C00678
Figure US20090181994A1-20090716-C00679
 CH3
Figure US20090181994A1-20090716-C00680
Figure US20090181994A1-20090716-C00681
 CH3
Figure US20090181994A1-20090716-C00682
Figure US20090181994A1-20090716-C00683
 CH3
Figure US20090181994A1-20090716-C00684
Figure US20090181994A1-20090716-C00685
 CH3
Figure US20090181994A1-20090716-C00686
Figure US20090181994A1-20090716-C00687
 CH3
Figure US20090181994A1-20090716-C00688
Figure US20090181994A1-20090716-C00689
 CH3
Figure US20090181994A1-20090716-C00690
Figure US20090181994A1-20090716-C00691
 CH3
Figure US20090181994A1-20090716-C00692
Figure US20090181994A1-20090716-C00693
 CH3
Figure US20090181994A1-20090716-C00694
Figure US20090181994A1-20090716-C00695
 CH3
Figure US20090181994A1-20090716-C00696
Figure US20090181994A1-20090716-C00697
 CH3
Figure US20090181994A1-20090716-C00698
Figure US20090181994A1-20090716-C00699
 CH3
Figure US20090181994A1-20090716-C00700
Figure US20090181994A1-20090716-C00701
 CH3
Figure US20090181994A1-20090716-C00702
Figure US20090181994A1-20090716-C00703
 CH3
Figure US20090181994A1-20090716-C00704
Figure US20090181994A1-20090716-C00705
 CH3
Figure US20090181994A1-20090716-C00706
Figure US20090181994A1-20090716-C00707
 CH3
Figure US20090181994A1-20090716-C00708
Figure US20090181994A1-20090716-C00709
 CH3
Figure US20090181994A1-20090716-C00710
Figure US20090181994A1-20090716-C00711
 CH3
Figure US20090181994A1-20090716-C00712
Figure US20090181994A1-20090716-C00713
 CH3
Figure US20090181994A1-20090716-C00714
Figure US20090181994A1-20090716-C00715
 CH3
Figure US20090181994A1-20090716-C00716
Figure US20090181994A1-20090716-C00717
 CH3
Figure US20090181994A1-20090716-C00718
Figure US20090181994A1-20090716-C00719
 CH3
Figure US20090181994A1-20090716-C00720
Figure US20090181994A1-20090716-C00721
 CH3
Figure US20090181994A1-20090716-C00722
Figure US20090181994A1-20090716-C00723
 CH3
Figure US20090181994A1-20090716-C00724
Figure US20090181994A1-20090716-C00725
 CH3
Figure US20090181994A1-20090716-C00726
Figure US20090181994A1-20090716-C00727
 CH3
Figure US20090181994A1-20090716-C00728
Figure US20090181994A1-20090716-C00729
 CH3
Figure US20090181994A1-20090716-C00730
Figure US20090181994A1-20090716-C00731
 CH3
Figure US20090181994A1-20090716-C00732
Figure US20090181994A1-20090716-C00733
 CH3
Figure US20090181994A1-20090716-C00734
Figure US20090181994A1-20090716-C00735
 CH3
Figure US20090181994A1-20090716-C00736
Figure US20090181994A1-20090716-C00737
 CH3
Figure US20090181994A1-20090716-C00738
Figure US20090181994A1-20090716-C00739
 CH3
Figure US20090181994A1-20090716-C00740
Figure US20090181994A1-20090716-C00741
 CH3
Figure US20090181994A1-20090716-C00742
Figure US20090181994A1-20090716-C00743
 CH3
Figure US20090181994A1-20090716-C00744
Figure US20090181994A1-20090716-C00745
 CH3
Figure US20090181994A1-20090716-C00746
Figure US20090181994A1-20090716-C00747
 CH2CH3
Figure US20090181994A1-20090716-C00748
Figure US20090181994A1-20090716-C00749
 CH2CH3
Figure US20090181994A1-20090716-C00750
Figure US20090181994A1-20090716-C00751
 CH2CH3
Figure US20090181994A1-20090716-C00752
Figure US20090181994A1-20090716-C00753
 CH2CH3
Figure US20090181994A1-20090716-C00754
Figure US20090181994A1-20090716-C00755
 CH2CH3
Figure US20090181994A1-20090716-C00756
Figure US20090181994A1-20090716-C00757
 CH2CH3
Figure US20090181994A1-20090716-C00758
Figure US20090181994A1-20090716-C00759
Figure US20090181994A1-20090716-C00760
Figure US20090181994A1-20090716-C00761
Figure US20090181994A1-20090716-C00762
 CH3
Figure US20090181994A1-20090716-C00763
Figure US20090181994A1-20090716-C00764
 CH3
Figure US20090181994A1-20090716-C00765
Figure US20090181994A1-20090716-C00766
Figure US20090181994A1-20090716-C00767
Figure US20090181994A1-20090716-C00768
Figure US20090181994A1-20090716-C00769
 CH3
Figure US20090181994A1-20090716-C00770
Figure US20090181994A1-20090716-C00771
 CH3
Figure US20090181994A1-20090716-C00772
Figure US20090181994A1-20090716-C00773
 CH3
Figure US20090181994A1-20090716-C00774
Figure US20090181994A1-20090716-C00775
 CH3
Figure US20090181994A1-20090716-C00776
Figure US20090181994A1-20090716-C00777
 CH3
Figure US20090181994A1-20090716-C00778
Figure US20090181994A1-20090716-C00779
 CH3
Figure US20090181994A1-20090716-C00780
Figure US20090181994A1-20090716-C00781
 CH3
Figure US20090181994A1-20090716-C00782
Figure US20090181994A1-20090716-C00783
 CH3
Figure US20090181994A1-20090716-C00784
Figure US20090181994A1-20090716-C00785
 CH3
Figure US20090181994A1-20090716-C00786
Figure US20090181994A1-20090716-C00787
 CH3
Figure US20090181994A1-20090716-C00788
Figure US20090181994A1-20090716-C00789
 CH3
Figure US20090181994A1-20090716-C00790
Figure US20090181994A1-20090716-C00791
 CH3
Figure US20090181994A1-20090716-C00792
Figure US20090181994A1-20090716-C00793
 CH3
Figure US20090181994A1-20090716-C00794
Figure US20090181994A1-20090716-C00795
 CH3
Figure US20090181994A1-20090716-C00796
Figure US20090181994A1-20090716-C00797
 CH3
Figure US20090181994A1-20090716-C00798
Figure US20090181994A1-20090716-C00799
 CH3
Figure US20090181994A1-20090716-C00800
Figure US20090181994A1-20090716-C00801
 CH3
Figure US20090181994A1-20090716-C00802
Figure US20090181994A1-20090716-C00803
 CH3
Figure US20090181994A1-20090716-C00804
Figure US20090181994A1-20090716-C00805
 CH3
Figure US20090181994A1-20090716-C00806
Figure US20090181994A1-20090716-C00807
 CH3
Figure US20090181994A1-20090716-C00808
Figure US20090181994A1-20090716-C00809
 CH3
Figure US20090181994A1-20090716-C00810
Figure US20090181994A1-20090716-C00811
 CH3
Figure US20090181994A1-20090716-C00812
Figure US20090181994A1-20090716-C00813
 CH3
Figure US20090181994A1-20090716-C00814
Figure US20090181994A1-20090716-C00815
 CH3
Figure US20090181994A1-20090716-C00816
Figure US20090181994A1-20090716-C00817
 CH3
Figure US20090181994A1-20090716-C00818
Figure US20090181994A1-20090716-C00819
 CH3
Figure US20090181994A1-20090716-C00820
Figure US20090181994A1-20090716-C00821
 CH3
Figure US20090181994A1-20090716-C00822
Figure US20090181994A1-20090716-C00823
 CH3
Figure US20090181994A1-20090716-C00824
Figure US20090181994A1-20090716-C00825
 CH3
Figure US20090181994A1-20090716-C00826
Figure US20090181994A1-20090716-C00827
 CH3
Figure US20090181994A1-20090716-C00828
 CH3 CH3
Figure US20090181994A1-20090716-C00829
Figure US20090181994A1-20090716-C00830
 CH3
Figure US20090181994A1-20090716-C00831
 H CH3
Figure US20090181994A1-20090716-C00832
 H CH3
Figure US20090181994A1-20090716-C00833
 H CH3
Figure US20090181994A1-20090716-C00834
 H CH3
Figure US20090181994A1-20090716-C00835
 H CH3
Figure US20090181994A1-20090716-C00836
Figure US20090181994A1-20090716-C00837
 CH3
Figure US20090181994A1-20090716-C00838
Figure US20090181994A1-20090716-C00839
 CH3
Figure US20090181994A1-20090716-C00840
Figure US20090181994A1-20090716-C00841
 CH3
Figure US20090181994A1-20090716-C00842
Figure US20090181994A1-20090716-C00843
 CH3
Figure US20090181994A1-20090716-C00844
Figure US20090181994A1-20090716-C00845
 CH3
Figure US20090181994A1-20090716-C00846
Figure US20090181994A1-20090716-C00847
 CH3
Figure US20090181994A1-20090716-C00848
Figure US20090181994A1-20090716-C00849
 CH3
Figure US20090181994A1-20090716-C00850
Figure US20090181994A1-20090716-C00851
 CH3
Figure US20090181994A1-20090716-C00852
Figure US20090181994A1-20090716-C00853
 CH3
Figure US20090181994A1-20090716-C00854
 CbzNH— CH3
Figure US20090181994A1-20090716-C00855
 NH2 CH3
Figure US20090181994A1-20090716-C00856
Figure US20090181994A1-20090716-C00857
 CH3
Figure US20090181994A1-20090716-C00858
Figure US20090181994A1-20090716-C00859
 CH3
Figure US20090181994A1-20090716-C00860
Figure US20090181994A1-20090716-C00861
 CH3
Figure US20090181994A1-20090716-C00862
Figure US20090181994A1-20090716-C00863
 CH3
Figure US20090181994A1-20090716-C00864
Figure US20090181994A1-20090716-C00865
 CH3
Figure US20090181994A1-20090716-C00866
Figure US20090181994A1-20090716-C00867
 CH3
Figure US20090181994A1-20090716-C00868
Figure US20090181994A1-20090716-C00869
 CH3
Figure US20090181994A1-20090716-C00870
Figure US20090181994A1-20090716-C00871
 CH3
Figure US20090181994A1-20090716-C00872
Figure US20090181994A1-20090716-C00873
 CH3
Figure US20090181994A1-20090716-C00874
Figure US20090181994A1-20090716-C00875
 CH3
Figure US20090181994A1-20090716-C00876
Figure US20090181994A1-20090716-C00877
 CH3
Figure US20090181994A1-20090716-C00878
Figure US20090181994A1-20090716-C00879
 CH3
Figure US20090181994A1-20090716-C00880
Figure US20090181994A1-20090716-C00881
 CH3
Figure US20090181994A1-20090716-C00882
Figure US20090181994A1-20090716-C00883
 CH3
Figure US20090181994A1-20090716-C00884
Figure US20090181994A1-20090716-C00885
 CH3
Figure US20090181994A1-20090716-C00886
Figure US20090181994A1-20090716-C00887
 CH3
Figure US20090181994A1-20090716-C00888
Figure US20090181994A1-20090716-C00889
 CH3
Figure US20090181994A1-20090716-C00890
Figure US20090181994A1-20090716-C00891
 CH3
Figure US20090181994A1-20090716-C00892
and structural formula III, or a pharmaceutically acceptable salt thereof
(III)
Figure US20090181994A1-20090716-C00893
 R5′ R1 Cl
Figure US20090181994A1-20090716-C00894
 Cl
Figure US20090181994A1-20090716-C00895
 Cl
Figure US20090181994A1-20090716-C00896
 Cl
Figure US20090181994A1-20090716-C00897
 Cl
Figure US20090181994A1-20090716-C00898
 F
Figure US20090181994A1-20090716-C00899
 F
Figure US20090181994A1-20090716-C00900
 F
Figure US20090181994A1-20090716-C00901
or a pharmaceutically acceptable salt thereof.
6. A method in accordance with claim 5, wherein the compound administered is selected from the group consisting of:
Figure US20090181994A1-20090716-C00902
Figure US20090181994A1-20090716-C00903
or a pharmaceutically acceptable salt thereof.
7. A method in accordance with claim 5, wherein the compound administered is selected from the group consisting of
Figure US20090181994A1-20090716-C00904
or a pharmaceutically acceptable salt thereof.
8. A method of reducing the risk of developing cognitive impairment in a mammalian patient in need thereof comprising administering to the patient an effective amount of a compound selected from the group consisting of structural formula I:
Figure US20090181994A1-20090716-C00905
or a pharmaceutically acceptable salt thereof; wherein
each p is independently 0, 1, or 2;
each n is independently 0, 1, or 2;
X is selected from the group consisting of a single bond, O, S(O)p, NR6,
Figure US20090181994A1-20090716-C00906
R1 is selected from the group consisting of
arylcarbonyl,
(CH2)n-aryl, and
(CH2)n-heteroaryl;
in which aryl and heteroaryl are unsubstituted or substituted with one to three substituents independently selected from R5;
R2 is selected from the group consisting of
hydrogen,
C1-8 alkyl,
C2-6 alkenyl, and
(CH2)n—C3-6 cycloalkyl;
in which alkyl, alkenyl, and cycloalkyl are unsubstituted or substituted with one to three substituents independently selected from R8 and oxo;
each R4 is independently selected from the group consisting of hydrogen,
halogen,
hydroxy,
oxo,
C1-3 alkyl, and
C1-3 alkoxy;
R3 is selected from the group consisting of
hydrogen,
C1-10 alkyl
C2-10 alkenyl,
(CH2)n—C3-6 cycloalkyl,
(CH2)n-aryl, and
(CH2)n-heteroaryl;
(CH2)n-heterocyclyl;
in which aryl, heteroaryl and heterocyclyl are unsubstituted or substituted with one to three substituents independently selected from R5; and alkyl, alkenyl, and cycloalkyl are unsubstituted or substituted with one to five groups independently selected from R8 and oxo;
R5 and R8 are independently selected from the group consisting of
hydrogen,
formyl,
C1-6 alkyl,
(CH2)n-aryl,
(CH2)n-heteroaryl,
(CH2)n-heterocyclyl,
(CH2)nC3-7 cycloalkyl,
halogen,
OR7,
(CH2)nN(R7)2,
cyano,
(CH2)nCO2R7,
NO2,
(CH2)nNR7SO2R6,
(CH2)nSO2N(R7)2,
(CH2)nS(O)pR6,
(CH2)nSO20R7,
(CH2)nNR7C(O)N(R7)2,
(CH2)nC(O)N(R7)2,
(CH2)nNR6C(O)R6,
(CH2)nNR6CO2R7,
O(CH2)nC(O)N(R7)2,
CF3,
CH2CF3,
OCF3,
OCHCF2, and
OCH2CF3;
wherein aryl, heteroaryl, cycloalkyl, and heterocyclyl are unsubstituted or substituted with one to three substituents independently selected from halogen, hydroxy, C1-4 alkyl, trifluoromethyl, trifluoromethoxy, and C1-4 alkoxy; and wherein any methylene (CH2) carbon atom in R5 and R8 is unsubstituted or substituted with one to two groups independently selected from halogen, hydroxy, and C1-4 alkyl; or two substituents when on the same methylene (CH2) carbon atom are taken together with the carbon atom to which they are attached to form a cyclopropyl group;
each R6 is independently selected from the group consisting of
C1-8 alkyl,
(CH2)n-aryl,
(CH2)n-heteroaryl, and
(CH2)nC3-7 cycloalkyl;
wherein alkyl and cycloalkyl are unsubstituted or substituted with one to five substituents independently selected from halogen, oxo, C1-4 alkoxy, C1-4 alkylthio, hydroxy, amino; and aryl and heteroaryl are unsubstituted or substituted with one to three substituents independently selected from cyano, halogen, hydroxy, amino, carboxy, trifluoromethyl, trifluoromethoxy, C1-4 alkyl, and C1-4 alkoxy;
or two R6 groups together with the atom to which they are attached form a 5- to 8-membered mono- or bicyclic ring system optionally containing an additional heteroatom selected from O, S, and NC1-4 alkyl; and
each R7 is hydrogen or R6;
structural formula II, or a pharmaceutically acceptable salt thereof
(II)
Figure US20090181994A1-20090716-C00907
 R3 R2 R1
Figure US20090181994A1-20090716-C00908
 CH3
Figure US20090181994A1-20090716-C00909
Figure US20090181994A1-20090716-C00910
 CH3
Figure US20090181994A1-20090716-C00911
Figure US20090181994A1-20090716-C00912
 CH3
Figure US20090181994A1-20090716-C00913
Figure US20090181994A1-20090716-C00914
 CH3
Figure US20090181994A1-20090716-C00915
Figure US20090181994A1-20090716-C00916
 CH3
Figure US20090181994A1-20090716-C00917
Figure US20090181994A1-20090716-C00918
 CH3
Figure US20090181994A1-20090716-C00919
Figure US20090181994A1-20090716-C00920
 CH3
Figure US20090181994A1-20090716-C00921
Figure US20090181994A1-20090716-C00922
 CH3
Figure US20090181994A1-20090716-C00923
Figure US20090181994A1-20090716-C00924
 CH3
Figure US20090181994A1-20090716-C00925
Figure US20090181994A1-20090716-C00926
 CH3
Figure US20090181994A1-20090716-C00927
Figure US20090181994A1-20090716-C00928
 CH3
Figure US20090181994A1-20090716-C00929
Figure US20090181994A1-20090716-C00930
 CH3
Figure US20090181994A1-20090716-C00931
Figure US20090181994A1-20090716-C00932
 CH3
Figure US20090181994A1-20090716-C00933
Figure US20090181994A1-20090716-C00934
 CH3
Figure US20090181994A1-20090716-C00935
Figure US20090181994A1-20090716-C00936
 CH3
Figure US20090181994A1-20090716-C00937
Figure US20090181994A1-20090716-C00938
 CH3
Figure US20090181994A1-20090716-C00939
Figure US20090181994A1-20090716-C00940
 CH3
Figure US20090181994A1-20090716-C00941
Figure US20090181994A1-20090716-C00942
 CH3
Figure US20090181994A1-20090716-C00943
Figure US20090181994A1-20090716-C00944
 CH3
Figure US20090181994A1-20090716-C00945
Figure US20090181994A1-20090716-C00946
 CH3
Figure US20090181994A1-20090716-C00947
Figure US20090181994A1-20090716-C00948
 CH3
Figure US20090181994A1-20090716-C00949
Figure US20090181994A1-20090716-C00950
 CH3
Figure US20090181994A1-20090716-C00951
Figure US20090181994A1-20090716-C00952
 CH3
Figure US20090181994A1-20090716-C00953
Figure US20090181994A1-20090716-C00954
 CH3
Figure US20090181994A1-20090716-C00955
Figure US20090181994A1-20090716-C00956
 CH3
Figure US20090181994A1-20090716-C00957
Figure US20090181994A1-20090716-C00958
 CH3
Figure US20090181994A1-20090716-C00959
Figure US20090181994A1-20090716-C00960
 CH3
Figure US20090181994A1-20090716-C00961
Figure US20090181994A1-20090716-C00962
 CH3
Figure US20090181994A1-20090716-C00963
Figure US20090181994A1-20090716-C00964
 CH3
Figure US20090181994A1-20090716-C00965
Figure US20090181994A1-20090716-C00966
 CH3
Figure US20090181994A1-20090716-C00967
Figure US20090181994A1-20090716-C00968
 CH3
Figure US20090181994A1-20090716-C00969
Figure US20090181994A1-20090716-C00970
 CH3
Figure US20090181994A1-20090716-C00971
Figure US20090181994A1-20090716-C00972
 CH3
Figure US20090181994A1-20090716-C00973
Figure US20090181994A1-20090716-C00974
 CH3
Figure US20090181994A1-20090716-C00975
Figure US20090181994A1-20090716-C00976
 CH3
Figure US20090181994A1-20090716-C00977
Figure US20090181994A1-20090716-C00978
 CH3
Figure US20090181994A1-20090716-C00979
Figure US20090181994A1-20090716-C00980
 CH3
Figure US20090181994A1-20090716-C00981
Figure US20090181994A1-20090716-C00982
 CH3
Figure US20090181994A1-20090716-C00983
Figure US20090181994A1-20090716-C00984
 CH3
Figure US20090181994A1-20090716-C00985
Figure US20090181994A1-20090716-C00986
 CH3
Figure US20090181994A1-20090716-C00987
Figure US20090181994A1-20090716-C00988
 CH3
Figure US20090181994A1-20090716-C00989
Figure US20090181994A1-20090716-C00990
 CH3
Figure US20090181994A1-20090716-C00991
Figure US20090181994A1-20090716-C00992
 CH3
Figure US20090181994A1-20090716-C00993
Figure US20090181994A1-20090716-C00994
 CH3
Figure US20090181994A1-20090716-C00995
Figure US20090181994A1-20090716-C00996
 CH3
Figure US20090181994A1-20090716-C00997
Figure US20090181994A1-20090716-C00998
 CH3
Figure US20090181994A1-20090716-C00999
Figure US20090181994A1-20090716-C01000
 CH3
Figure US20090181994A1-20090716-C01001
Figure US20090181994A1-20090716-C01002
 CH3
Figure US20090181994A1-20090716-C01003
Figure US20090181994A1-20090716-C01004
 CH3
Figure US20090181994A1-20090716-C01005
Figure US20090181994A1-20090716-C01006
 CH3
Figure US20090181994A1-20090716-C01007
Figure US20090181994A1-20090716-C01008
 CH3
Figure US20090181994A1-20090716-C01009
Figure US20090181994A1-20090716-C01010
 CH3
Figure US20090181994A1-20090716-C01011
Figure US20090181994A1-20090716-C01012
 CH3
Figure US20090181994A1-20090716-C01013
Figure US20090181994A1-20090716-C01014
 CH3
Figure US20090181994A1-20090716-C01015
Figure US20090181994A1-20090716-C01016
 CH3
Figure US20090181994A1-20090716-C01017
Figure US20090181994A1-20090716-C01018
 CH3
Figure US20090181994A1-20090716-C01019
Figure US20090181994A1-20090716-C01020
 CH3
Figure US20090181994A1-20090716-C01021
Figure US20090181994A1-20090716-C01022
 CH3
Figure US20090181994A1-20090716-C01023
Figure US20090181994A1-20090716-C01024
 CH3
Figure US20090181994A1-20090716-C01025
Figure US20090181994A1-20090716-C01026
 CH3
Figure US20090181994A1-20090716-C01027
Figure US20090181994A1-20090716-C01028
 CH3
Figure US20090181994A1-20090716-C01029
Figure US20090181994A1-20090716-C01030
 CH3
Figure US20090181994A1-20090716-C01031
Figure US20090181994A1-20090716-C01032
 CH3
Figure US20090181994A1-20090716-C01033
Figure US20090181994A1-20090716-C01034
 CH3
Figure US20090181994A1-20090716-C01035
Figure US20090181994A1-20090716-C01036
 CH3
Figure US20090181994A1-20090716-C01037
Figure US20090181994A1-20090716-C01038
 CH3
Figure US20090181994A1-20090716-C01039
Figure US20090181994A1-20090716-C01040
 CH2CH3
Figure US20090181994A1-20090716-C01041
Figure US20090181994A1-20090716-C01042
 CH2CH3
Figure US20090181994A1-20090716-C01043
Figure US20090181994A1-20090716-C01044
 CH2CH3
Figure US20090181994A1-20090716-C01045
Figure US20090181994A1-20090716-C01046
 CH2CH3
Figure US20090181994A1-20090716-C01047
Figure US20090181994A1-20090716-C01048
 CH2CH3
Figure US20090181994A1-20090716-C01049
Figure US20090181994A1-20090716-C01050
 CH2CH3
Figure US20090181994A1-20090716-C01051
Figure US20090181994A1-20090716-C01052
Figure US20090181994A1-20090716-C01053
Figure US20090181994A1-20090716-C01054
Figure US20090181994A1-20090716-C01055
 CH3
Figure US20090181994A1-20090716-C01056
Figure US20090181994A1-20090716-C01057
 CH3
Figure US20090181994A1-20090716-C01058
Figure US20090181994A1-20090716-C01059
Figure US20090181994A1-20090716-C01060
Figure US20090181994A1-20090716-C01061
Figure US20090181994A1-20090716-C01062
 CH3
Figure US20090181994A1-20090716-C01063
Figure US20090181994A1-20090716-C01064
 CH3
Figure US20090181994A1-20090716-C01065
Figure US20090181994A1-20090716-C01066
 CH3
Figure US20090181994A1-20090716-C01067
Figure US20090181994A1-20090716-C01068
 CH3
Figure US20090181994A1-20090716-C01069
Figure US20090181994A1-20090716-C01070
 CH3
Figure US20090181994A1-20090716-C01071
Figure US20090181994A1-20090716-C01072
 CH3
Figure US20090181994A1-20090716-C01073
Figure US20090181994A1-20090716-C01074
 CH3
Figure US20090181994A1-20090716-C01075
Figure US20090181994A1-20090716-C01076
 CH3
Figure US20090181994A1-20090716-C01077
Figure US20090181994A1-20090716-C01078
 CH3
Figure US20090181994A1-20090716-C01079
Figure US20090181994A1-20090716-C01080
 CH3
Figure US20090181994A1-20090716-C01081
Figure US20090181994A1-20090716-C01082
 CH3
Figure US20090181994A1-20090716-C01083
Figure US20090181994A1-20090716-C01084
 CH3
Figure US20090181994A1-20090716-C01085
Figure US20090181994A1-20090716-C01086
 CH3
Figure US20090181994A1-20090716-C01087
Figure US20090181994A1-20090716-C01088
 CH3
Figure US20090181994A1-20090716-C01089
Figure US20090181994A1-20090716-C01090
 CH3
Figure US20090181994A1-20090716-C01091
Figure US20090181994A1-20090716-C01092
 CH3
Figure US20090181994A1-20090716-C01093
Figure US20090181994A1-20090716-C01094
 CH3
Figure US20090181994A1-20090716-C01095
Figure US20090181994A1-20090716-C01096
 CH3
Figure US20090181994A1-20090716-C01097
Figure US20090181994A1-20090716-C01098
 CH3
Figure US20090181994A1-20090716-C01099
Figure US20090181994A1-20090716-C01100
 CH3
Figure US20090181994A1-20090716-C01101
Figure US20090181994A1-20090716-C01102
 CH3
Figure US20090181994A1-20090716-C01103
Figure US20090181994A1-20090716-C01104
 CH3
Figure US20090181994A1-20090716-C01105
Figure US20090181994A1-20090716-C01106
 CH3
Figure US20090181994A1-20090716-C01107
Figure US20090181994A1-20090716-C01108
 CH3
Figure US20090181994A1-20090716-C01109
Figure US20090181994A1-20090716-C01110
 CH3
Figure US20090181994A1-20090716-C01111
Figure US20090181994A1-20090716-C01112
 CH3
Figure US20090181994A1-20090716-C01113
Figure US20090181994A1-20090716-C01114
 CH3
Figure US20090181994A1-20090716-C01115
Figure US20090181994A1-20090716-C01116
 CH3
Figure US20090181994A1-20090716-C01117
Figure US20090181994A1-20090716-C01118
 CH3
Figure US20090181994A1-20090716-C01119
Figure US20090181994A1-20090716-C01120
 CH3
Figure US20090181994A1-20090716-C01121
 CH3 CH3
Figure US20090181994A1-20090716-C01122
Figure US20090181994A1-20090716-C01123
 CH3
Figure US20090181994A1-20090716-C01124
 H CH3
Figure US20090181994A1-20090716-C01125
 H CH3
Figure US20090181994A1-20090716-C01126
 H CH3
Figure US20090181994A1-20090716-C01127
 H CH3
Figure US20090181994A1-20090716-C01128
 H CH3
Figure US20090181994A1-20090716-C01129
Figure US20090181994A1-20090716-C01130
 CH3
Figure US20090181994A1-20090716-C01131
Figure US20090181994A1-20090716-C01132
 CH3
Figure US20090181994A1-20090716-C01133
Figure US20090181994A1-20090716-C01134
 CH3
Figure US20090181994A1-20090716-C01135
Figure US20090181994A1-20090716-C01136
 CH3
Figure US20090181994A1-20090716-C01137
Figure US20090181994A1-20090716-C01138
 CH3
Figure US20090181994A1-20090716-C01139
Figure US20090181994A1-20090716-C01140
 CH3
Figure US20090181994A1-20090716-C01141
Figure US20090181994A1-20090716-C01142
 CH3
Figure US20090181994A1-20090716-C01143
Figure US20090181994A1-20090716-C01144
 CH3
Figure US20090181994A1-20090716-C01145
Figure US20090181994A1-20090716-C01146
 CH3
Figure US20090181994A1-20090716-C01147
 CbzNH— CH3
Figure US20090181994A1-20090716-C01148
 NH2 CH3
Figure US20090181994A1-20090716-C01149
Figure US20090181994A1-20090716-C01150
 CH3
Figure US20090181994A1-20090716-C01151
Figure US20090181994A1-20090716-C01152
 CH3
Figure US20090181994A1-20090716-C01153
Figure US20090181994A1-20090716-C01154
 CH3
Figure US20090181994A1-20090716-C01155
Figure US20090181994A1-20090716-C01156
 CH3
Figure US20090181994A1-20090716-C01157
Figure US20090181994A1-20090716-C01158
 CH3
Figure US20090181994A1-20090716-C01159
Figure US20090181994A1-20090716-C01160
 CH3
Figure US20090181994A1-20090716-C01161
Figure US20090181994A1-20090716-C01162
 CH3
Figure US20090181994A1-20090716-C01163
Figure US20090181994A1-20090716-C01164
 CH3
Figure US20090181994A1-20090716-C01165
Figure US20090181994A1-20090716-C01166
 CH3
Figure US20090181994A1-20090716-C01167
Figure US20090181994A1-20090716-C01168
 CH3
Figure US20090181994A1-20090716-C01169
Figure US20090181994A1-20090716-C01170
 CH3
Figure US20090181994A1-20090716-C01171
Figure US20090181994A1-20090716-C01172
 CH3
Figure US20090181994A1-20090716-C01173
Figure US20090181994A1-20090716-C01174
 CH3
Figure US20090181994A1-20090716-C01175
Figure US20090181994A1-20090716-C01176
 CH3
Figure US20090181994A1-20090716-C01177
Figure US20090181994A1-20090716-C01178
 CH3
Figure US20090181994A1-20090716-C01179
Figure US20090181994A1-20090716-C01180
 CH3
Figure US20090181994A1-20090716-C01181
Figure US20090181994A1-20090716-C01182
 CH3
Figure US20090181994A1-20090716-C01183
Figure US20090181994A1-20090716-C01184
 CH3
Figure US20090181994A1-20090716-C01185
and structural formula III, or a pharmaceutically acceptable salt thereof
(III)
Figure US20090181994A1-20090716-C01186
 R5′ R1 Cl
Figure US20090181994A1-20090716-C01187
 Cl
Figure US20090181994A1-20090716-C01188
 Cl
Figure US20090181994A1-20090716-C01189
 Cl
Figure US20090181994A1-20090716-C01190
 Cl
Figure US20090181994A1-20090716-C01191
 F
Figure US20090181994A1-20090716-C01192
 F
Figure US20090181994A1-20090716-C01193
 F
Figure US20090181994A1-20090716-C01194
or a pharmaceutically acceptable salt thereof.
9. A method in accordance with claim 8, wherein the compound administered is selected from the group consisting of:
Figure US20090181994A1-20090716-C01195
Figure US20090181994A1-20090716-C01196
or a pharmaceutically acceptable salt thereof.
10. A method in accordance with claim 8, wherein the compound administered is selected from the group consisting of
Figure US20090181994A1-20090716-C01197
or a pharmaceutically acceptable salt thereof.
11. A method according to claim 2, wherein the cognitive impairment is dementia.
12. A method according to claim 11, wherein the dementia is Alzheimer's disease.
13. A method according to claim 5, wherein the cognitive impairment is dementia.
14. A method according to claim 13, wherein the dementia is Alzheimer's disease.
15. A method according to claim 8, wherein the cognitive impairment is dementia.
16. A method according to claim 15, wherein the dementia is Alzheimer's disease.
US12/364,902 2002-12-20 2009-02-03 Triazole derivatives as inhibitors of 11-beta-hydroxysteroid dehydrogenase-1 Abandoned US20090181994A1 (en)

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