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AU7179781A - Therapeutically useful tetralin derivatives - Google Patents

Therapeutically useful tetralin derivatives

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AU7179781A
AU7179781A AU71797/81A AU7179781A AU7179781A AU 7179781 A AU7179781 A AU 7179781A AU 71797/81 A AU71797/81 A AU 71797/81A AU 7179781 A AU7179781 A AU 7179781A AU 7179781 A AU7179781 A AU 7179781A
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compound
formula
group
treatment
carbon atoms
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Folk Lars-Erik Arvidsson
Per Arvid Emil Carlsson
Uli Alf Hacksell
John Stephan Mikael Hjorth
Per Lennart Lindberg
John Lars Gunnar Nillson
Domingo Sanchez
Hakan Vilhelm Wikstrom
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Astra Lakemedel AB
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Astra Lakemedel AB
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Priority claimed from SE8004002A external-priority patent/SE8004002L/en
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  • Acyclic And Carbocyclic Compounds In Medicinal Compositions (AREA)

Description

THERAPEUTICALLY USEFUL TETRALIN DERIVATIVES
DESCRIPTION
Technical Field
The present invention is related to new 1,2,3,4-tetra hydro-2-naphtylamines, to processes for preparing such compounds, pharmaceutical preparation of such compounds and the use of such compounds in therapy.
An object of the invention is to provide compounds for therapeutic use, especially compounds having a therapeutic activity in the central nervous system. A further object is to provide compounds having an effect on the 5-hydroχy tryptamine neurones in mammals including man.
Background Art
Compounds of the formula
are disclosed by a number of references. Thus, Mc Dermed et al. (J. Fled. Chem. 18, 362 (1975)) describe i.a. compounds wherein YI and YII are 7-OH and 8-0H, respectively, and RI and RII are both methyl or both propyl and wherein YI and YII are 5-0H and 8-OH, respectively, and RI and RII together are -C2H4-O-C2H4-. Said compounds are indicated to have dopaminergic properties although certain compounds are reported, to be inactive. Further Me Dermed et al. (J. Fled. Chem.19, 547, (1976)) describe dopaminergic compounds of formula I
.above, wherein YI is 5-OH, 6-OH or 7-OH, YII is H and RI and RII are both propyl. Rusterholz et al. (3. Fled. Chem. 19, 99, (1976)) describe compounds of formula I, wherein YI is 5-0H or 5-0CH3, YII is 8-0H or 8-0CH3 and RI and RII are selected from H and methyl. Some of said compounds are potent prolactin inhibitors and believed to be dopamine agonists.
Cannon et al. (3. Fled. Chem. 20, 1111, (1977)) have studied dopaminergic effects of a number of 5,6- and 6,7-dihydroxy compounds according to formula I.
Ames et al. (3. Chem. Soc. 2636 (1965)) disclose the preparation of a large number of compounds, among which are those of formula I above-wherein YI is H and YII is a methoxy, ethoxy, n- or iso-propoxy, or n-, sek- or tert- butoxy group in the 5 or 8 position and R I and RII are H or alkyl groups having 1-4 carbon atoms. The compounds are indicated to be prepared for pharmacological testing.
However, no utility or pharmacological activity is yet known for the compounds just mentioned.
Disclosure of invention
According to the present invention it has been found that novel compounds of the formula
wherein Y is OH, NH2, R3COO, R3CONH or CH3SO2NH and R3 is an alkyl group having 1 to 5 carbon atoms, a benzyl or phenyl group, and R I is an alkyl group having 1 to 8 carbon atoms, a benzyl or phenethyl group and R 2 is hydrogen or an alkyl group having 1 to 5 carbon atoms or R1 and R2 together form an alkylene group having 4 to 6 carbon atoms, as well as pharmaceutically acceptable acid addition salts thereof, possess unexpected pharmacological properties rendering them useful in therapy and fulfilling the objects stated above. Processes for preparation of such compounds, their pharmaceutical and medical use and pharmaceutical preparations and methods of treatment employing such compounds constitute further aspects of the invention.
Compounds of formula Ila below wherein Ya is OCH3, are intermediates in preparation of the corresponding hydroxy compounds of formula II. According to the invention said compounds are found to have valuable therapeutic properties. Thus, according to a further aspect the invention is related to the pharmaceutical and medical use of compounds as well as to pharmaceutical preparations and methods of treatment employing compounds of the formula
wherein Ya is OCH3, OH, NH2, R3COO, R3CONH or CH3SO2NH and R 1 , R 2 and R 3 are as defined above, as well as pharmaceutically acceptable acid addition salts thereof.
Both organic and inorganic acids can be employed to form non-toxic pharmaceutically acceptable acid addition salts of the compounds of this invention. Illustrative acids are sulfuric, nitric, phosphoric, hydrochloric, citric, acetic, lactic, tartaric, pamoic, ethanedisulfonic, sulfamic, succinic, cyclohexylsulfamic, fumaric, maleic and benzoic acid. These salts are readily prepared by methods known in the art. According to a preferred embodiment the invention is related to compounds of the formula II wherein Y is OH or
R3COO. Further preferred are compounds wherein R1 and R2 are the same or different and selected from ethyl and n- propyl. For their medical use application further compounds of formula Ila wherein Y represents CH3O belong to the preferred group of compounds.
The compounds of formula II and Ila contain an asymmetric carbon atom in the aliphatic ring moiety, i.e. the ring carbon atom adjacent to the nitrogen atom. The therapeutic properties of the compounds may to a greater or lesser degree be ascribed to either or both of the two enantiomers occurring. Thus the pure enantiomers as well as mixtures thereof are within the scope of the invention.
The invention takes into consideration that compounds which structurally deviates from the formula II or Ila after administration to a living organism may be transformed to a compound of the formula II or Ila and in this structural form exert their effects. Likewise, certain compounds of formula II or Ila may be metabolized into other compounds of formula II before exerting their effect.
Compounds of the invention wherein Y or Ya is R1COO, R1CONH or CH3SO2NH are thus believed to exert their main activity after metabolism to compounds wherein Y or Ya is OH, NH2 and NH2, respectively.
Flethods of Preparation
The compounds of the invention may be obtained by one of the following methods constituting a further aspect of the invention. a ) An ether of the formu la
wherein R represents a hydrocarbon residue, preferably an alkyl group having 1-5 carbon atoms, or a benzyl group, and R 1 and R2 are as defined above, may be cleaved to form a compound of formula II wherein Y is a hydroxy group.
The cleavage may be carried out by treating the compound of formula III with an acidic nucleophilic reagent such as aqueous HBr, or HI, HBr/CH3COOH, BBr3, AICI3, pyridine-HCl or (CH3)3SiI, with a basic nucleophilic reagent such as
CH3C6H4-SΘ or C2H5-SΘ.
When Ra is a benzyl group the cleavage may also be carried out by reduction, preferably with hydrogen using Pd or PtO2 as catalyst.
b) A compound of formula II wherein Y is OH or NH2 and R2 is other than H may be converted into a compound of the same formula wherein Y is R1COO, R1CONH or CH3SO2NH by treating the firstmentioned compound with an appropriate carboxylic acid halide R1COX or anhydride (R1CO)2O or with a methy lsulfonyl halide CH3SO2X in the presence of a base such as triethy lamine or pyridine or an acid such as H2SO4 or CF3COOH, X represents a halogen, preferably Cl or Br.
c) A compound of formula IV
wherei n Rb i s ei t he r R1 or R2 , and R1 R2 and
Ya are as defined above, may be converted into a compound of formula II wherein Y is OH, by alkylation of the nitrogen atom with an appropriate alkylating agent. Thus, the starting compound wherein Rb is R2 may be treated with an alkyl, benzyl or phenethyl halide or tosylate R1 X1 , wherein
X1 represents Cl, Br, I or in an organic solvent such as acetonitrile or acetone and in the presence of a base such as K2CO3 or NaOH, or said starting compound may be treated with a carboxylic acid NaBH4 complex RcCOOHNaBH4, wherein Rc is defined by the relation Rc-CH2- equals R1. To the formation of a compound of formula I wherein at least one of R1 and R2 is CH3, the alkylation reaction may be carried out by treatment of the compound of formula IV with a formaldehyde - Na(CN)BH3 mixture, or with formaldehyde and formic acid. To the formation of a compound of formula II wherein R1 is a cycloalkyl group, the alkylation may be carried out by reaction of the compound of formula IV wherein Rb is R2 with a cyclic ketone of the formula wherein n is 1, 2, or 3, whereby the intermediate of formula
formed, is reduced, preferably with hydrogen using Pd or PtO2 as catalyst. d) An amide of the formula.
wherein Yais CH3O, OH or NH2, Rd is an alkyl group defined by the relation Rd-CH2- equals either R1 or R2 and Re is the other of R1 and R2, may be reduced, e.g. by treatment with a hydride reducing agent such as LiAlH. in ether or tetrahydrofuran or BH3 in tetrahydrofuran, to the formation of a compound of formula II or Ila.
e) A compound of the formula
may be reduced to the corresponding amine. When the starting material is an isomeric mixture as regards the position of the nitro group chromatographic separation either before or after the reduction yields the 8-amino compound of formula II. The reduction is suitably carried out with hydrogen and Pd catalyst.
f ) A compound of the formu la
wherein Ya and Rb are as defined above, may be catalytically reduced to the formation of a compound of formula IV. With appropriate meanings of Ya and Rb the product obtained also satisfies formula II or Ila. Said method is especially useful in preparation of pure enantiomers as enantiomer separation of the benzyl derivatives of formula XIV may easily be done by recrystallizat ion with optically active tartaric acid.
g) An enamine with either a C1-C2 or a C2-C3, double bond or an imine base (without R ) or immonium salt (e.g. C104 or BF4 ) with a C2-N double bond of the formula
wherein Ya, R1 and R 2 are as defined above may be reduced to a compound of formula II or Ila, preferably by catalytic hydrogenation using PtO2 or Pd as a catalyst. h) A compound of the formula
wherein M1 and M2 are the same or different and each represents is a group sensitive to hydrogenolysis such as hydroxy in benzylic position or halogen, and R 1 and R2 are as defined above, may be converted to a compound of formula II or Ila by reduction.
Thus, a keto function may be either directly converted to
CH2 by treatment with e.g. hydrazine under alkaline conditions or by a stepwise reduction by using e.g. catalytic hydrogenation which may involve an intermediary formation of a hydroxy group and, where possible, also an elimination to a double bond. Reduction of a group may be carried out by using a nucleophilic hydride reducing agent such as LiAlH4, or catalytic hydrogenation.
i) In a compound of the formula
wherein X represents SO3H, Cl or NH2, a hydroxy group may be substituted for the group X to the formation of a compound of formula II wherein Y represents a hydroxy group When X is SO3H or Cl said reaction may be carried out by treatment with a strong alkali under heating, suitably with an alkali melt such as KOH when X is SO3H, and with a strong aqueous alkali such as NaOH or KOH when X is Cl. When X is NH2 the reaction may be carried out by treatment with aqueous nitrous acid to the formation of an intermediate diazonium compound which is then subjected to hydrolysis in water.
Free bases formed may subsequently be converted into their acid addition salts, and acid addition salts formed may subsequently be converted into the corresponding bases or other acid addition salts.
Preparation of Starting Flaterials
Starting materials for the methods of preparation described above may be obtained by several methods known in the art or described below.
A) The starting material for method a) according to formula III above may be prepared by one of the following methods:
A1)
A compound of formula VI is reacted with an amine such as ReNH2 in the presence of acetic acid and molecular sieves or methylamine hydrochloride in the presence of NaOH to the formation of an intermediate imine, which is reduced by catalytic hydrogenation to a compound of formula VII. When a tertiary amine is desired, compound VII is then acylated with a carboxylic acid chloride in the presence of triethylamine and subsequently reduced in the manner described under d) above to a compound of formula III. A compound of formula
III wherein R2 is H is obtainable directly from the amination of VI to VII. A2 )
For the preparation of a starting material wherein R1 is a cycloalkyl group, a compound of formula VI may be reacted with an azacycloalkane of the formula
wherein n is 1, 2, or 3 and the intermediate is catalytically hydrogenated suitably with Pt02 as the catalyst.
B) The starting materials for method b) are also compounds of the invention and are obtainable by a suitable method described under a), c), d), or e) above.
C) The starting materials for method c) are obtainable by a method analogous to the steps VI » VII of method A1) The hydrocarbon residue Ra is suitably split off from the compound of formula VII. when Ya =OH is desired in the compound of formula IV. Starting materials satisfying formula II or Ila are also obtainable by one of methods a) or d). D ) The starting materials for method d) are obtainable
D1) by steps of method A1 when in compound V Ya is. CH3O. When Ya is OH the starting compound is obtainable D2) by splitting off the hydrocarbon residue Ra in compound VIII, suitably with BBr3. When Y is NH2 the starting compound is obtainable D3) by reduction of a compound of the formula
in a manner analogous to method e) involving chromatographic separation. The compound X is obtainable by the reactions
The compound XII is prepared from XI in analogy with steps of method A1). Compound X is then obtained by treatment with HNO3, H2SO4 and water.
E) Starting materials for method e) are obtainable by amination of a compound of formula XI. The amination may be carried out in analogy with method A1 or A2 above. In the intermediate of formula
formed a nitro group is then introduced in analogy with the reaction according to 03 above. F) Starting materials of formula XIV employed accordingto method f) are obtainable by one of the above methods.
Pharmaceutical preparations
Pharmaceutical preparations of the compounds of the invention constitute a further aspect of the invention.
In clinical practice the compounds of the present invention will normally be administered orally, rectally, or by injection, in the form of pharmaceutical preparations comprising the active ingredient either as a free base or as a pharmaceutically acceptable non-toxic, acid addition salt, e.g. the hydrochloride, lactate, acetate, sulfamate, and the like, in association with a pharmaceutically acceptable carrier.
Accordingly, terms relating to the novel compounds of this invention, whether generically or specifically, are intended to include both the free amine base and the acidaddition salts of the free base, unless the context in which such terms are used, e.g. in the specific examples, would be inconsistent with the broad concept. The carrier may be a solid, semisolid or liquid diluent or capsule. These pharmaceutical preparations constitute a further aspect of this invention. Usually the active substance will constitute between 0.1 and 99% by weight of the preparation, more specifically between 0.5 and 20% by weight for preparations intended for injection and between 0.2 and 50% by weight for preparations suitable for oral administration.
Pharmaceutical preparations containing a compound of the invention may preferably contain between 2 and 50% by weight of the active substance, in such preparations the selected compound may be mixed with a solid fine grain carrier, e.g. lactose, saccharose, sorbitol, mannitol, starches such as potato starch, corn starch or amylopectin, cellulose derivatives, or gelatin and a lubricant such as magnesium stearate, calcium stearate, polyethylene glycol waxes, and the like, and then compressed to form tablets. If coated ta-blets are required, the cores, prepared as described above, may.be coated with a concentrated sugar solution which may contain, e.g. gum arabic, gelatin, talcum, titanium dioxide, and the like. Alternatively the tablet can be coated with a lacquer dissolved in a readily volatile organic solvent or mixture of organic solvents. Dyestuffs may be added to these coatings in order to readily distinguish between tablets containing different active substances or different amounts of the active compound.
For the preparation of soft gelatin capsules (pearl-shaped closed capsules) consisting of gelatin and, for example, glycerol, or similar closed capsules, the active substance may be admixed with a vegetable oil. Hard gelatin capsules may contain granulates of the active substance in combination with solid, fine grain carriers such as lactose, saccharose, sαrbitαl, mannitol, starches (e.g. potato starch, corn starch or amylopectin), cellulose derivatives or gelatin.
Liquid preparations for oral application may be in the form of syrups or suspensions, for example, solutions containing from about 0.2% to about 20% by weight of the active substance herein described, the balance being sugar and a mixture of ethanol, water, glycerol and propyleneglycol. Optionally such liquid preparations may contain colouring agents, flavouring agents, saccharine and carboxymethylcellulose as a thickening agent.
Solutions for parenteral applications by injection can be prepared in an aqueous solution of a water-soluble pharmaceutically acceptable salt of the active substance preferably in a concentration of from about 0.5% to about 10% by weight. These solutions may also contain stabilizing agents and/or buffering agents and may conveniently be provided in various dosage unit ampoules. In therapeutical treatment the suitable daily doses of the compounds of the invention are 1-2000 mg for oral application, preferentially 50-500 mg, and 0.1-100 mg for parenteιral application, preferentially 0.5-50 mg .
Working examples
The following examples will further illustrate the invention
Preparation of intermediates and compounds of formula Ila wherein_Ya_is_CH3O
Example II: 2-(n-propylamino)-8-methoxytetralin (Flethod Al)
To a solution of 8-methoxy-2-t et ra lo n e (10.2 g, 58 mmol) in absolute ethanol (175 ml) over 4 A molecular sieves (19.0 g) were added n-propy lamine (10.3 g, 174 mmol) and acetic acid (10.4 g,. 174 mmol). The mixture was shaken in a closed flask (N2 atmosphere) for half an hour, heated to 70oC and allowed to cool. The molecular sieves were filtered off, and the solution was hydrogenated catalytically over PtO2 at atmospheric pressure. After filtration and evaporation, the acetate of the title compound was washed with ether, and made alkaline with saturated Na2CO3 solution. The aqueous phase was extracted with ether and the combined organic layers were evaporated. The residue was passed through an alumina column with ether as eluant, precipitated as the hydrochloride and recrystallized from ethanol/ether.
Example I2. 2-(di-n-propylamino)-8-methoxytetralin (Flethod A1)
Propioπy lchloride (5.4 g, 58 mmol) in dry toluene (10 ml) was slowly added at 5oC to a solution of. 2-(propylamino)- 8-methoxytetralin (8.5 g, 39 mmol), triethylamine (5.9 g, 58 mmol) and dry toluene (60 ml). The mixture was stirred at room temperature for 30 min, whereupon the triethyl ammonium chloride formed was filtered off and the solventevaporated. The residue was passed through an alumina column with ether/light petroleum as eluant. After evaporation the amide dissolved in dry tetrahydrofuran (30 ml) was. added to a suspension of LiAIH4 (2.0 g, 53 mmol) in dry tetrahydrofuran (100 ml) under nitrogen. After stirring under reflux for 5 h, the mixture was hydrαlyzed, the precipitate was filtered off, and the solvent was evaporated. The residue was passed through an alumina column with ether/ /light petroleum (1+2), and the title compound was precipitated as the hydrochloride and recrystallized from sthanol/ether.
Example 13. 2-piperidino-8-methoxytetraliπ (Flethod A2)
A solution of 8-methoxy-2-tetralone (10.0 g, 57 mmol), piperidine (14.5 g, 170 mmol), and p-tolueπesulfonic acid (0.5 g) in dry toluene (500 ml) was refluxed for 24 h. The solvent was evaporated and the residue was dissolved in absolute ethanol and transferred to a Parr flask. Pt02 (0.5 g) was added and the hydrogenation was performed at 0.38 MPa gauge. The catalyst was filtered off, the solvent was evaporated, and the residue was passed through an alumina column with ether/light petroleum (1+1) as eluant. The title compound was precipitated as the hydrochloride and recrystallized from ethanol.
Example 14. 2-(methylamino)-8-methoxytetralin (Flethod A1)
8-methoxy-2-tetralone (5.0 g, 28 mmol) was dissolved in ethanol under nitrogen. Flethylamine hydrochloride (3.8 g, 56 mmol) dissolved in water (50 ml) and NaOH (5.6 g, 140 mmol), were added under stirring. After stirring for 20 min, the mixture was poured onto ice (100 g) mixed with concentrated HC1 (30 ml).. The acidic solution was hydrogenated catalytic ally over PtO2 (150 mg) in a Parr apparatus at 0.34 MPa gauge. After filtration, the ethanol was evaporated, and the remaining aqueous phase was poured into water (100 ml), washed with ether and made alkaline. Extraction with ether and evaporation gave the crude solid amine, which was passed through an alumina column with ether as eluant. The title compound was precipitated as the hydrochloride and recrystallized from i-propanol/ether.
Example 15. 8-amino-2-(N-n-propy1-N-propiony1)amino tetralin (Flethod 03)
2- (N-n-propyl-N-propionyl)aminotetralin (59.9 g, 0.24 mol) (prepared according to Al from 2-tetralone in 86% yield) was dissolved in CH3NO2 (1000 ml). A mixture of concentrated HNO3 (16.5 ml), concentrated H2SO4 (213 ml) and water (35.4 ml) was added dropwise under cooling and thorough stirring maintaining the temperature between 0-10ºC. The mixture was stirred at 0ºC for another 2 hours and then poured onto ice-water (4 1) . Extraction with CH2C12, washing the organic phase with water, drying (Na2SO4) and evaporation of the solvent gave a crude oil (64.4 g) of an isomeric mixture of 5-, 6-, 7 - and 8-mononitro-2- (N-n propyl-N-propionyl) aminotetralin . The mixture was dissolved in ethanol (1200 ml). Acetic acid (50 ml) and 10% Pd/C (3 g) was added and the mixture was hydrogenated at 0.34 MPa gauge. catalyst was filtered off and the solvent evaporated giving a residual oil. The oil was dissolved in 1 M HC1 (500 ml), and the solution was extracted with ether. The ether phase was discarded, the aqueous phase was made alkaline (Na2CO3) and extracted with ether. The organic phase was dried (Na2SO4) and the solvent evaporated giving a crude oil (57 g) of an isomeric mixture of 5-, 6-, 7- and 8-moήoamino-2-(N-n-propyl-N-propionyl) aminotetralin. A small amount (1.0 g) of the last-mentioned isomeric mixture was converted to the hydrochloride and chromatographed on an RP-18 column using MeoH-2 M NaOAc (1:1) + 2 % HOAc as eluant. (In this way all the isomers could be separated). The last fraction (a total volume of about 1000 ml), containing the pure β-isomer (HPLC), was worked up by first evaporating off the methanol, making the residual solution_ alkaline with 20 % NaOH and extracting with ether. The ether phase was dried (Na2SO.) and the solvent evaporated giving a residue (80 mg) of the desired product 8-amino-2-(N-n-propyl-N-propionyl)aminotetralin (NMR) .
Examplε 16. ( + ) -2-benzylamino-8-methoxytetralin
(+)-Tartaric acid (15.92 g, 0.106 mol) dissolved in hot ethanol (500 ml) was added to a hot solution of (±)-2--benzylamino-8-methoxytetralin (28.36 g, 0.106 mol) in ethanol (1500 ml). The solution was allowed to stand over night at room temperature. The crystals thus formed was recrystallized four times by dissolving in boiling ethanol and cooling to room temperature. The resolved amine was released with NaOH solution into ether. The organic layer was dried (K2CO3) and the solvent was removed under reduced pressure yielding ( + ) -2-benzylamino-8-methoxytetralin. A small sample was converted to the hydrochloride for analysis, melting point and determination of specific rotation.
The enantiomeric purity of the amine was determined by analysis of the NMR-spectrum of its O-methy Imandelamide which was prepared as follows: R ( - ) -2-Methoxy-2-phenylacetyl-chloride (155 mg, 0.8 mmol] dissolved in dry benzene (5 ml) was added to an ice-cooled solution of ( + ) -2-benzylamino- 8-methoxytetralin (150 mg, 0.6 mmol) and triethylamine (170 mg, 1.7 mmol) in dry benzene (20 ml). The mixture was stirred at room temperature for 1 hour whereupon it was fit.ltered and the solvent evaporated. The residue, dissolved in ether, was washed with 2N HCl, 2N NaOH and water. After drying (K2CO3) the organic layer the ether was distilled off and the crude amide was dissolved in dimethylsulfoxide-d6. In the nmr-spectrum of the diastereomeric amides the methin proton alpha to the methoxygroup gave singlets with different chemical shifts (5.36 and 5...44 ppm) . The enantiomeric purity was determined to more than 93 % by estimation of the relative areas under these peaks .
Example 17. ( + ) -2-propylaminp-8-methoxytetralin (Flethod F)
The hydrochloride of (+ ) -2-(N-n-benzyl-N-n-propylamino)- 8-methoxytetralin, prepared from (+)-2-benzylamino-8-methoxytetralin (3.65 g, 13.65 mmol) according to method A1, d, (Example 12), was dissolved in methanol (100 ml): Pd on charcoal catalyst was added and hydrogenolysis was performed at atmospheric pressure. Removal of catalyst and solvent gave ( + ) -2-propylamino-8-methoxytetralin as the hydrochloride, which was treated with 2N NaOH. The free amine was extracted with ether. The ether layer was removed, dried (K2CO3) and evaporated. The amine was purified on an alumina column with ether as eluant and converted to its hydrochloride and recrystallized from ethanol/ether.
Preparation_of_end_compounds_of_formula_II
Example El. 2-(di-n-propylamino)-8-hydroxytetralin hydrobromide (Flethod a)
2- (di-n-propylamino)-8-methoxytetralin hydrochloride (4.5 g) were suspended in 48 % HBr (100 ml). The mixture was then heated at 120ºC for 2 h under nitrogen. The hydrobromic acid was evaporated, water was added and evaporated. The residue was recrystallized from ethanol yielding the pure 2- (di-n-propylamino)-8-hydroxytetralin hydrobromide.
Example E2. 8-amino-2-di-n-propylaminotetralin hydro chloride (Method d)
8-amino-2-(N-n-propyl-N-propiony1)aminotetralin (80 mg, 0.31 mmol) dissolved in dry ether (10 ml) was added dropwise to a stirred mixture of LiAlH4 (0.2 g) in dry ether (10 ml) (N2 atmosphere) and then the mixture was stirred for 30 min at room temperature. Addition of water (0.2 ml), 15 % NaOH (0.2 ml) and finally water (0.6 ml) followed by filtration, drying (Na2SO4) of the filtrate and evaporation of the ether gave the product base as a residual oil (90 mg) (NMR) .
The base was converted to the hydrochloride by dissolving in ether and precipitating with HCl-saturated ether. The hydrochloride was recrystallized from ethanol-ether.
According to the methods of the Examples above the following compounds were prepared and recrystallized as acid addition salts from ethanol/ether or isolated as the bases.
Footnotes to the preceding table
a) All salts, except for compound 25, were submitted for elemental" analysis (C, H, N); All the analyses were satisfactory.
b) NMR δ(CDCl3) 0.9.3H, t), 1.15.3H, t), 1.4-3.7(15H, m], 6.35-6.7(2H, m), 6.95(1H, t)
c) Measured in methanol, enantiomeric purity >93%
d) Yield from theoretical amount of isomer in racemate
e) Compound 2 as starting material.
f) Compound 6 as starting material.
g) NMR δ(CDC13) 0.89 (6H, t), 1.44 (4H, m) , 1.2-2.2 C2H, m), 2.27 (3H, s), 2.47 (4H, t), 2.3-3.1 (5H, m), 6,7-7.26 (3H, m) .
The following examples illustrate how the compounds of formula II or Ila employed according to the present invention may be included into pharmaceutical preparations.
Examplε PI. Preparation of soft gelatine capsules
500 g of active substance are mixed with 500 g of corn oil, whereupon the mixture is filled in soft gelatine capsules, each capsule containing 100 mg of the mixture (i.e. 50 mg of active substance).
Example P2. Preparation of tablets
0.5 kg of active substance are mixed with 0.2 kg of silicic acid of the trade mark Aerosil. 0.45 kg of potato starch and 0.5 kg of lactose are mixed therewith and the mixture is moistened with a starch paste prepared from 50 g of potato starch and distilled water, whereupon the mixture is granulated through a sieve. The granulate is dried and sieved, whereupon 20 g of magnesium stearate are mixed into it. Finally the mixture is pressed into tablets each weighing 172 mg.
Example P3. Preparation of a syrup
100 g of active substance are dissolved in 300 g of 95 % ethanol, whereupon 300 g of glycerol, aroma and colouring agents (q.s.) and 1000 ml of water are mixed therein. A syrup is obtained.
Example P4. Preparation of an injection solution
Active substance (hydrobromide) (1 g), sodiumchlαride (0.8 g) and ascorbic acid (0.1 g) are dissolved in sufficient amount of distilled water to give 100 ml of solution. This solution, which contains 10 mg of active substance per ml, is used in filling ampoules, which are sterilized by heating at 120°C for 20 minutes.
Pharmacology
Pharmacological_treatment_of_degression_in_man
Evidence is available that in depressed patients the neurotransmission in the central nervous system (CNS) may be disturbed. These disturbances appear to involve the neurotransmitters noradrenaline (NA) and 5-hydroxytryptamine (5-HT). The drugs most frequently used in the treatment of depression are considered to act by improving the neurotransmission of either or both of these phsyiological agonists. Available data suggest that the enhancement of 5-HT neurotransmission will primarily improve the depressed mood and anxiety, whereas the enhancement of noradrenaline neurotransmissio.n will rather improve the retardation symptoms occurring in depressed patients. In recent years many efforts have been made to develop new drugs with high selectivity for the imprαvement of the 5-HT neurotransmission in the CNS.
The mechanism of action for the drugs generally used today in the therapy of mental depression is indirect, i.e. they act. by blocking the reuptake of the neurotransmitters (NA and/or 5-HT) released from nerve terminals in the CNS, thus increasing the concentration of these transmitters in the synaptic cleft and hence restoring an adequate neurotransmission. The new antidepressive agent (Z)-Dimethyl-amino-1-(4-bromophenyl)-1-(3-pyridyl)propene (zimelidine) with documented good clinical effects is believed to act as such a reuptake inhibitor with high selectivity for 5-HT neurons . A fundamentally different way to improve the neurotransmission in the central 5-HT-neurons would be to use a direct 5-HT-receptor agonist. In order to minimize side effects, a high selectivity for this kind of receptors wouid then be preferable.
While searching for new dopamine (DA) -receptor agonists, we surprisingly found that a group of compounds of the formula II and Ila instead had a selective, direct stimulating effect on central 5-HT receptors.
In order to evaluate the 5-HT-receptor stimulating effect and selectivity, the compounds were tested both behaviourally and biochemically.
Behavioural and biochemical activity in reserpine-pretreated rats.
a. Antagonism of the reserpine-induced "neuroleptic syndrome" in the rat (gross behaviour).
Depletion of the monoamine stores with reserpine brings about a "neuroleptic syndrome" characterized by hypomotility catalepsy, muscle rigidity, hunch-backed posture as well as a number of other central and peripheral signs of monoamine depletion. The whole or parts of this syndrome can be reversed by the administration of drugs that stimulate DA or 5-HT receptors directly or indirectly.
Stimulation of the DA receptors (e.g. with apomorphine) gives rise to both locomotion and stereotyped behaviour such as sniffing, gnawing and jumping. On the other hand, stimulation of the 5-HT receotors [e.g. with 5-hydroxytrvotophan (5-HTP) combined with MAO-inhibitors], gives rise to a very different behaviour. The animals lie flat on the cage floor exhibiting forward movements with extended forepaws padding ("piano-playing") and abducted hindlegs, occasionally with some tremor in the fαrebody and with Straubtail (stiff tail i.a.) reaction.
b. In-vivo determination of rat brain tyrosine and tryptophan hydroxylation after reserpine pretreatment (biochemical DA- and 5-HT receptor activity).
The compounds under evaluation were tested biochemically for central DA- and 5-HT-receptor (pre- and/or postsynaptic) stimulating activity. The concept of this biochemical screening method is that a DA- or 5-HT-receptor agonist will stimulate the receptor and through regulatory feedback systems effect a decline-in tyrosine or tryptophan hydroxylating activity, respectively, and a subsequent reduction in the synthesis rate for DA and 5-HT in the presynaptic neuron. Dopa and 5-HTP formation, as determined after in-vivo inhibition of the aromatic L-amino acid decarboxylase with NSD 1015 (3-hydroxybenzylhydrazine hydrochloride) are taken as indirect measures of DA- and 5-HT-synthesis rates, respectively.
Analogous conditions probably exist also for central NA-neurons. Effects on the dopa formation in the NA-predominated hemispheral parts (mainly cortex) may thus be considered to reflect NA-receptor-mediated changes.
c. Experimental procedures.
Rats (150-300 g) pretreated with reserpine (5 mg/kg, 18 h before) were given the compounds under evaluation. Gross behavioural observations (changes in motility, hindleg abduction etc; c.f. above) were made. Subsequent administration of NSD 1015, decapitation, brain dissection [corpora striata, the limbic forebrain and the remaining hemispheral portions (mainly cortex) of rat brain], homogenization, centrifugat ion, ion-exchange chrαmatography and spectro-fluorimetric measurements (all as described in detail by Wikstrom et al., 3. Med. Chem., 21, 864-867, 1978 and references cited therein) gave the actual dopa and 5-HTP levels. Several doses (n=4-6.) were tested for each compound and brain area. The dose of a compound giving 70 % of the control 5-HTP level in the rat brain part was then estimated These values ( "ED70%" ) are presented in Table 1.
d. Results.
All the compounds in Table 1 were both behaviourally and biochemically active, producing the above mentioned effects indicating central 5-HT-receptor stimulation. The absenceof significant decreases in the dopa levels in the different brain parts suggests that none of the compounds possess central NA- or DA-receptor stimulating effects at the dosage under consideration.
The investigated compounds may be classified into 3 subgroups with regard to biochemical potency: 1) those with an "ED70%" between 0.01-1.0 μmol/kg such as compound 20 and compound 21 which are considered to be most advantageous for medical use, 2) those with an "ED70%." between 1.0-10 μmol/kg such as compounds 17 and 23 and 3) those with an "ED70%" above 10 μmol/kg such as compounds 18 and 10 which are considered to be of borderline interest. The resolved isomers were found to be about as potent as the corresponding racemates.
a) "ED
70: " represents the dose giving 70 % of the control 5-HTP level.
b] Similar values were obtained for all the brain parts [ths limbic forebrain, striatum and the hemispheral portions (mainly cortex)] investigated . c) None of the compounds tested gave any significant reduction in dopa formation in the brain parts investigated at doses 8 times the "ED70%". Effect on the sexual functions
Due to the strong and selective 5-HT-stimulating effect of the compounds of the invention, a few of these were also tested on the hetero-sexual behaviour in male rats. There is considerable evidence that central 5-HT receptor activation is involved in mediating the sexual behaviour.
During these pharmacological investigations it was revealed (see below) that the compounds of the invention have a very strong activity on the sexual behaviour in male rats, In the masculine mating pattern a marked (dose dependent) decrease was found in the number of intromissions as well as mounts preceding ejaculation, and in the ejaculatory latency, while the period of sexual inactivity following ejaculation was not significantly changed. The efficacy (maximal effect) in this respect for the compounds tested seems to be higher than for any other compound known (and tested).
It was (in preliminary experiments) further found that male rats rendered sexual inactive by castration became sexual active after treatment with compound 8.
Due to these qualities of the compounds of the invention, also a possible therapeutic application in the treatment of sexual disturbances may certainly be foreseen.
Exgerimental_grocedure
Male Wistar rats (12 months old; sexually experienced) were injected i.p. every second day in a balanced order with different doses of ths compounds dissolved in physiological saline and injected in a volume of 2 ml/kg. Testing was begun 15 min after the drug treatment. Mating arenas were 50 cm diameter acrylic glass cages with wood shavings on the floor. The stimulus females were of Wistar strain, primed with estradiol benzoate (20 μg/animal) 48 h prior to testing and progesterone (0.5 ml/animal) 4-6 h before testing.
The occurrence of mounts, intromissions and ejaculations were scored by an experienced observer. The measures of masculine copulatory behavior further included mount latency and intromission latency which are time from introduction of the stimulus female to the first mount and first intromission respectively. A copulatory series includes the mounts and intromissions preceding an ejaculation. Ejaculatory latency is the time from the first intromission in a copulatory series to the ejaculation terminating that series. The postej aculatory interval is the time from an ejaculation to the next intromission. Tests were terminated when the rat had achieved one ejaculation and started the second series of copulations, or, if the intromission latency was >15 min, the ejaculation latency was >30 min, or the postej aculatory interval was >15 min.
Results
a. Normal rats
Results obtained for racemic 2-diprαpylamino-8-methoxytetralin (compound 8), its resolved enantiomers (compounds (+)-8 and (-)-8) and 2-dipropylamino-8-hydroxytetralin (compound 20) are shown in Table 2. The resolved isomers were found to be about as potent as the corresponding racemates. b. Castrated rats (preliminary results)
Out of 9 castrated male rats treated with 8 mg/kg of racemic compound 8, 5 mounted the female, 2 of these 5 made intromissions and 1 of these 2 ejaculated, while none out of 9 saline-treated castrated animals showed any sexual activity.
Conclusion
The pharmacological data affirm that the compounds of the present invention are very potent centrally acting 5-HT-receptor stimulating agents with high selectivity. for 5-HT over DA and NA receptors. At present, no compound with such properties seems to be known in the literature. In addition to this, the compounds have stronger _effeet than any other known compound on the masculine sexual behaviour. Due to this unique pharmacological profile, the compounds are of great clinical interest in the treatment of certain disorders in the CNS such as depression and sexual disturbances. Additional potential uses of the new compounds are in the control of pain, where 5-HT has been shown to be involved, and in senile disturbances of movement and mental function e.g. senile dementia, where a decreased level of brain 5-HT has been demonstrated.
Best mode of carrying out the invention
The compound 2-(di-n-propylamino)-8-hydroxytetralin and its salts, processes for preparing said compound and methods employing said compound in therapy represent the best mode of carrying out the invention known to the inventors at present.

Claims

1. A compound of the formula
wherein Y is OH, NH2, R3COO, R3CONH or CH3SO2NH and R3 is an alkyl group having 1 to 5 carbon atoms, a benzyl or phenyl group, and R1 is an alkyl group having 1 to 8 carbon atoms, a benzyl or phenethyl group and R2 is hydrogen or an alkyl group having 1 to 5 carbon atoms or R 1 and R2 together form an alkylene group having 4 to
6 carbon atoms, as the bass or a pharmaceutically acceptable acid addition salt thereof.
2. A compound according to claim 1 wherein Y is OH or R3COO.
3. A compound according to claim 1 or 2 wherein R 1 and R2 are the same or different and selected from ethyl and n-propyl.
4. A compound for pharmaceutical or medical use characterized by the formula
wherein Ya is OCH3, OH, NH2, R3COO, R3CONH, or CH3SO2NH and R3 is an alkyl group having 1-5 carbon atoms, a benzyl or phenyl group, and R1 is an alkyl group having 1 to 8 carbon atoms, a benzyl or phenethyl group and R2 is hydrogen or an alkyl group having 1 to 5 carbon atoms or R1 and R2 together from an alkylene group having 4 to 6 carbon atoms as the base or a pharmaceutically acceptable acid addition salt thereof.
5. A compound according to claim 4 wherein Y is OCH3,
OH or R3COO.
6. A compound according to claim 5 wherein Y is OCH3
7. A compound according to either of claims 4 to 6 wherein R1 aanndd R2 aarrte the same or different and selected from ethyl and n-propyl
8. A process for preparing a compound of the formula
wherein Y is OH, NH2, R3COO, R3CONH or CH3SO2NH and R3 is an alkyl group having 1 to 5 carbon atoms, a benzyl or phenyl group, and R1 is an alkyl group having 1 to 8 carbon atoms, a benzyl or phenethyl group and R2 is hydrogen or an alkyl group having 1 to 5 carbon atoms or R1 and R2 together form an alkylene group having 4 to 6 carbon atoms, as the base or a pharmaceutically acceptable acid addition salt thereof, characterized in that a) an ether of the formula
whsrein Ra represents a hydrocarbon residue, and R1 and R2 are as defined above, is cleaved to form a compound of formula II wherein Y is a hydroxy group,
b) a compound of formula II wherein Y is OH or NH2 and R2 is other than H is converted into a compound of the same formula wherein Y is R1COO, R1CONH or CH3SO2NH by treating the firstment ioned compound with an appropriate carboxylic acid halide R COX or anhydride (R1CO)2O or with a methylsulfonyl halide CH3EO2X in ths presence of a base,
c) a compound of formula IV
wherein Rb is either R1 or R2 and R1 R 2 and Ya are as defined above, is converted into a compound of formula II wherein Y is OH, by alkylation of the nitrogen atom with an appropriate alkylating agent,
d) an amide of the formula
wherein Ya is OH or NH2, Rd is an alkyl group defined by the relation Rd-CH2- equals either R1 or R2 and Re is the other of R1 and R2, is reduced to the formation of a compound of formula II,
e) a compound of the formula
is reduced to the corresponding amine, and if required an isomeric mixture as regards the position of the nitro group is chromatographically separated either before or after the reduction to the formation of the 8-amino compound of formula II, or
f) a compound of the formula
wherein Ya and Rb are as defined above, is catalytically reduced to the formation of a compound of formula IV, g) an enamipe with either a C1- C2 or a C2--C3 double bond or an imine base (without R2) or immonium salt (e.g. C104 or BF4 ) with a C2-N double bond of the formula
wherein Ya, R1 and R2 are as defiπed above, is reduced to a compound of formula II or IIa,
h) a compound of the formula
one of M1 and M2 represents and the other represents -CH2 , is a group sensitive to hydrogenolysis such as OH in benzylic position or halogen, and R 1 and R2 are as defined above, is converted to a compound of formula II or Ila by reduction, or
i) a compound of the formula
wherein X represents SO3H, Cl or NH2, a hydroxy group is substituted for the group X to the formation of a compound of formula II wherein Y represents a hydroxy group;
whereupon optionally a base obtained is converted to a pharmaceutically acceptable acid addition salt or a salt obtained is converted to the base or to a different, pharmaceutically acceptable acid addition salt, and optionally an isomeric mixture obtained is separated to a pure isomer.
9. A pharmaceutical preparatioπ comprising as an active ingredient a compound according to claim 1 or claim 4, in conjunction with a pharmaceutically acceptable carrier.
10. A pharmaceutical preparation for the treatment of dis orders in ths central nervous system, comprising as an active ingredient a compound according to claim 1 or claim 4, in conjunction with a pharmaceutically acceptable carrier.
11. A method of treatment of disorders in the central nervous system, comprising administering to a host in need of treatment a therapeutically effective amount of a compound according to claim 1 or claim 4.
12. A method for treatment of depression, comprising administering to a host in need of treatment a therapeutically effective amount of a compound according to claim 1 or claim 4.
13. A method for treatment of sexual disturbances, comprising administering to a host in need of treatment a therapeutically effective amount of a compound according to claim 1 or claim 4.
14. A method for treatment of pain, comprising administering to a host in need of treatment a therapeutically ef'fective amount of a compound according to claim 1 or claim 4.
15. A method for treatment of senile dementia, comprising administering to a host in need of treatment a therapeutically effective amount of a compound according to claim 1 or claim 4.
16. Compounds, processes, pharmaceutical preparations and methods of treatment as claimed in any of claims 1-15, and substantially as described.
AU71797/81A 1980-05-29 1981-05-26 Therapeutically useful tetralin derivatives Abandoned AU7179781A (en)

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SE8004002A SE8004002L (en) 1980-05-29 1980-05-29 THERAPEUTICALLY APPLICABLE TETRALIN DERIVATIVES
SE8004002 1980-05-29
PCT/SE1981/000155 WO1981003491A1 (en) 1980-05-29 1981-05-26 Therapeutically useful tetralin derivatives

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Cited By (1)

* Cited by examiner, † Cited by third party
Publication number Priority date Publication date Assignee Title
AU572497B2 (en) * 1981-05-08 1988-05-12 Per Arvid Emil Carlsson 1,2,3,4-tetrahydro-2-naphthylamines

Cited By (1)

* Cited by examiner, † Cited by third party
Publication number Priority date Publication date Assignee Title
AU572497B2 (en) * 1981-05-08 1988-05-12 Per Arvid Emil Carlsson 1,2,3,4-tetrahydro-2-naphthylamines

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FI822226A0 (en) 1982-06-21
FI822226L (en) 1982-06-21

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