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DE1052982B - Process for the production of new, spasmolytically effective, basic ethers, their salts or quaternary ammonium compounds - Google Patents

Process for the production of new, spasmolytically effective, basic ethers, their salts or quaternary ammonium compounds

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Publication number
DE1052982B
DE1052982B DEA27439A DEA0027439A DE1052982B DE 1052982 B DE1052982 B DE 1052982B DE A27439 A DEA27439 A DE A27439A DE A0027439 A DEA0027439 A DE A0027439A DE 1052982 B DE1052982 B DE 1052982B
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endomethylene
mol
radical
salts
quaternary ammonium
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German (de)
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Phil Nat Habil Herbert Arno Dr
Dr Med Norbert Brock
Dr Phil Engelbert Kuehas
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CHEM FAB
Asta Medica GmbH
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CHEM FAB
Asta Werke AG Chemische Fabrik
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Priority to DEA27439A priority Critical patent/DE1052982B/en
Priority to CH876163A priority patent/CH374990A/en
Priority to CH6113858A priority patent/CH371112A/en
Publication of DE1052982B publication Critical patent/DE1052982B/en
Pending legal-status Critical Current

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    • CCHEMISTRY; METALLURGY
    • C07ORGANIC CHEMISTRY
    • C07DHETEROCYCLIC COMPOUNDS
    • C07D295/00Heterocyclic compounds containing polymethylene-imine rings with at least five ring members, 3-azabicyclo [3.2.2] nonane, piperazine, morpholine or thiomorpholine rings, having only hydrogen atoms directly attached to the ring carbon atoms
    • C07D295/04Heterocyclic compounds containing polymethylene-imine rings with at least five ring members, 3-azabicyclo [3.2.2] nonane, piperazine, morpholine or thiomorpholine rings, having only hydrogen atoms directly attached to the ring carbon atoms with substituted hydrocarbon radicals attached to ring nitrogen atoms
    • C07D295/08Heterocyclic compounds containing polymethylene-imine rings with at least five ring members, 3-azabicyclo [3.2.2] nonane, piperazine, morpholine or thiomorpholine rings, having only hydrogen atoms directly attached to the ring carbon atoms with substituted hydrocarbon radicals attached to ring nitrogen atoms substituted by singly bound oxygen or sulfur atoms
    • CCHEMISTRY; METALLURGY
    • C07ORGANIC CHEMISTRY
    • C07CACYCLIC OR CARBOCYCLIC COMPOUNDS
    • C07C35/00Compounds having at least one hydroxy or O-metal group bound to a carbon atom of a ring other than a six-membered aromatic ring
    • C07C35/22Compounds having at least one hydroxy or O-metal group bound to a carbon atom of a ring other than a six-membered aromatic ring polycyclic, at least one hydroxy group bound to a condensed ring system
    • C07C35/23Compounds having at least one hydroxy or O-metal group bound to a carbon atom of a ring other than a six-membered aromatic ring polycyclic, at least one hydroxy group bound to a condensed ring system with hydroxy on a condensed ring system having two rings
    • C07C35/28Compounds having at least one hydroxy or O-metal group bound to a carbon atom of a ring other than a six-membered aromatic ring polycyclic, at least one hydroxy group bound to a condensed ring system with hydroxy on a condensed ring system having two rings the condensed ring system containing seven carbon atoms

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  • Chemical & Material Sciences (AREA)
  • Organic Chemistry (AREA)
  • Pharmaceuticals Containing Other Organic And Inorganic Compounds (AREA)
  • Nitrogen Condensed Heterocyclic Rings (AREA)

Description

Verfahren zur Herstellung neuer, spasmolytisch wirksamer, basischer Äther, deren Salzen bzw. quaternären Ammoniumverbindungen Es ist bekannt, daß basische Äther der allgemeinen Formel I, in denen ein Benzolring durch den 2,5-Endomethylen-d 3-cyclohexenylrest gemäß der allgemeinen Formel II, in denen R1 und R2 Alkylreste bedeuten, die gegebenenfalls zusammen mit dem Stickstoffatom zu einem heterocyclischen Rest, z. B. einem Pyrrolidin-, Piperidin- oder Morpholinrest, verbunden sein können, ersetzt ist, starke, das Atropin übertreffende anticholinergische Wirkungen besitzen (vgl. die deutsche Patentschrift 955 595). Es wurde nun gefunden, daß Verbindungen der allgemeinen Formel III, in der R., und R, die obige Bedeutung haben, R3 für einen 2,5-Endomethylencyclohexyl- oder einen 2,5-Endomethylen-43-cyclohexenylrest steht, der gegebenenfalls in 6-Stellung durch einen niederen Alkyl rest substituiert sein kann, wobei R4 für Wasserstoff oder einen niederen Alkylrest steht, wenn R3 ein 6-Alkyl-2,5-endomethylen-43-cyclohexenylrest ist, und R4 für Alkyl steht, wenn R3 ein 2,5-Endomethylen-43-cyclohexenylrest ist und X für Wasserstoff oder Halogen steht, überraschenderweise eine weitgehende Änderung des pharmakologischen Wirkspektrums aufweisen. Die Verbindungen der allgemeinen Formel III können gegebenenfalls im Endomethylenring hydriert sein.Process for the production of new, spasmolytically active, basic ethers, their salts or quaternary ammonium compounds It is known that basic ethers of the general formula I, in which a benzene ring is separated by the 2,5-endomethylene-d 3-cyclohexenyl radical according to the general formula II , in which R1 and R2 are alkyl radicals which, optionally together with the nitrogen atom, form a heterocyclic radical, e.g. B. a pyrrolidine, piperidine or morpholine radical, can be connected, is replaced, have strong anticholinergic effects exceeding atropine (cf. German Patent 955 595). It has now been found that compounds of the general formula III, in which R., and R, have the above meaning, R3 stands for a 2,5-endomethylene cyclohexyl or a 2,5-endomethylene-43-cyclohexenyl radical, optionally in 6-position can be substituted by a lower alkyl radical, where R4 is hydrogen or a lower alkyl radical when R3 is a 6-alkyl-2,5-endomethylene-43-cyclohexenyl radical, and R4 is alkyl when R3 is a 2 , 5-endomethylene-43-cyclohexenyl radical and X stands for hydrogen or halogen, surprisingly have an extensive change in the pharmacological spectrum of activity. The compounds of the general formula III can optionally be hydrogenated in the endomethylene ring.

Die neuen Verbindungen können erhalten werden, indem man ein Carbinol der allgemeinen Formel in der R3, R4 und X die vorerwähnte Bedeutung haben, in an sich bekannter Weise mit Verbindungen der allgemeinen Formel in der R1 und R2 die vorerwähnte Bedeutung haben und Hal für ein Halogenatom steht, kondensiert, die erhaltenen Aminoäther oder deren Hydrierungsprodukte in die entsprechenden Salze physiologisch unbedenklicher Säuren überführt bzw. durch Umsetzung zeit Alkylestern, z. B. Alkylhalogeniden oder Dialkylsulfaten, in üblicher Weise quaternisiert.The new compounds can be obtained by making a carbinol of the general formula in which R3, R4 and X have the aforementioned meaning, in a manner known per se with compounds of the general formula in which R1 and R2 have the aforementioned meaning and Hal stands for a halogen atom, condensed, the amino ethers obtained or their hydrogenation products converted into the corresponding salts of physiologically acceptable acids or by reaction time alkyl esters, eg. B. alkyl halides or dialkyl sulfates, quaternized in the usual way.

Die als Ausgangsstoffe verwendeten Carbinole werden aus den entsprechenden Aldehyden bzw. Ketonen durch Grignard-Reaktion in an sich bekannter Weise erhalten.The carbinols used as starting materials are made from the corresponding Aldehydes or ketones obtained by Grignard reaction in a manner known per se.

Die therapeutischen Eigenschaften der neuen Verbindungen im Vergleich zu den vorbekannten Verbindungen ergeben sich aus der nachfolgenden Tabelle. Wenn man die Werte- der zu vergleichenden Substanzen prüft, ergibt sich; daB die Substanzen a), b) und.-c) in Bestätigung der- Angaben in der deutschen .Patentschrift 955 595 eine- das Atropin um das 2- bis 3fache übersteigende. Wirkung besitzen, während die Wirkung beim myotropen Krampf nur ein Fünftel bis ein Zehntel -der Wirkung . des Papaverins ausmacht. Es handelt sich dabei somit urn typische Anticholinergica.The therapeutic properties of the new compounds in comparison with the previously known compounds are shown in the table below. If you check the values of the substances to be compared, you get; that the substances a), b) and.-c) in confirmation of the information in the German patent specification 955 595 one which exceeds atropine by 2 to 3 times. Have an effect, while the effect in myotropic spasm is only a fifth to a tenth of the effect. of papaverine. These are therefore typical anticholinergics.

. Im Gegensatz hierzu. zeigen die neuen, von der allgemeinen Formel III abgeleiteten Verbindungen eine ausgeprägte und gesteigerte- Papaverinwirkung. Gegenüber Papaverin ist dieser Effekt um -das 2- bis 8fache, gegenüber den vorbekannten Vergleichssubstanzen im Extremfall um das 80fache gesteigert. Dabei ist die anticholinergische Wirkkomponente ähnlich stark entwickelt wie bei den vorbekannten Vergleichssubstanzen.. In contrast to this. show the new, from the general formula III derived compounds have a pronounced and increased papaverine effect. Compared to papaverine, this effect is 2 to 8 times greater than the previously known ones In extreme cases, comparison substances increased by 80 times. Here is the anticholinergic Active component similarly developed as with the previously known comparison substances.

Die nachfolgenden Beispiele` erläutern die Erfindung. Beispiel l ,B-Dimethylaminoäthyl-(6-methyl-2,5-endomethylend 3-tetrahydrobenzhydryl)-äther Eine Lösung von 53,5 g (0,25 Mol) 6-Methyl-2,5-endomethylen-4 3-tetrahydrobenzhydrol in 250 ml Toluol wird unter Rühren mit 10 g (0,25- Mol) Natriumamid versetzt. Nach 15 Minuten werden 27 g (0,25 Mol) Dimethylaminoäthylchlorid zugegeben und das Gemisch 2'-/2 Stunden zum Sieden erhitzt. Nach dem Erkalten wird es mit Wasser aufgenommen. und der organische Anteil mit verdünnter Salzsäure ausgeschüttelt. Die salzsaure Lösung wird mit Natronlauge alkalisch gemacht und ausgeäthert. Nach dem Trocknen über Natriumsulfat wird der Äther entfernt und der Rückstand im Vakuum fraktioniert destilliert. Kp.o,,, = 132 bis 135°C; Ausbeute 50 bis 60°/o der Theorie; Hydrochlorid: F. = -123 bis 127° C.The following examples explain the invention. Example 1, B-Dimethylaminoethyl- (6-methyl-2,5-endomethylend 3-tetrahydrobenzhydryl) ether A solution of 53.5 g (0.25 mol) of 6-methyl-2,5-endomethylene-4 3-tetrahydrobenzhydrol in 250 ml of toluene is while stirring with 10 g (0.25 mol) of sodium amide are added. After 15 minutes, 27 g (0.25 mol) of dimethylaminoethyl chloride are added added and the mixture heated to boiling for 2 '- / 2 hours. After it has cooled down it was taken up with water. and the organic part extracted with dilute hydrochloric acid. The hydrochloric acid solution is made alkaline with sodium hydroxide solution and extracted with ether. To After drying over sodium sulfate, the ether is removed and the residue is removed in vacuo fractionally distilled. Bp = 132 to 135 ° C; Yield 50 to 60% of theory; Hydrochloride: F. = -123 to 127 ° C.

28,5 g (0,1 Mol) des ß-Dimethylaminoäthyl-(6-methyl-2,5-endomethylen-43-tetrahydrobenzhydryl)-äthers werden in 75 ml Essigsäureäthylester gelöst und mit 14,2 g (0,1 Mol) Methyljodid versetzt. Nach 24.-Stunden werden 250 ml absoluter Äther zugegeben, das ausgefallene Salz abgesaugt und aus Aceton oder Essigsäureäthylester umgelöst. .F. = 175 bis 184°C; Ausbeute: 50 bis 600/, der Theorie.28.5 g (0.1 mol) of ß-dimethylaminoethyl (6-methyl-2,5-endomethylene-43-tetrahydrobenzhydryl) ether are dissolved in 75 ml of ethyl acetate and 14.2 g (0.1 mol) Methyl iodide added. After 24 hours, 250 ml of absolute ether are added, the precipitated salt is filtered off with suction and redissolved from acetone or ethyl acetate. .F. = 175 to 184 ° C; Yield: 50 to 600 /, of theory.

Aus 28,5 g (0,1 Mol) ß-DimethylaminoäthyI-(6-methyl-2,5-endomethylen-43-tetrahydrobenzhydryl)-äther und 15,6 g (0,1 Mol) Äthyljodid wird in analoger Weise das ß - Dimethylaminoäthyl- (6 @methyl -2,5 - endomethylen -43-tetrahydrobenzhydryl)-ätherjodäthylat hergestellt. F. = 118 bis 126°C; Ausbeute: 55 bis 65°/o der Theorie. Beispie12 ß-Diäthylaminoäthyl-(6-methyl-2,5-endomethylen-4 3-tetrahydrobenzhydryl)-äther Aus 53,5 g (0,25 Mol) 6-Methyl-2,5-endomethylen-4 3-tetrahydrobenzhydrol und 34 g (0,25 Mol) Diäthylaminoäthylchlorid erhält man in analoger Weise wie im Beispiel 1 den ß-Diäthylaminoäthyl-(6-methyl-2,5-endomethylen-43-tetrahydrobenzhydryl)-äther. Kp.o,4 = 136 bis 139°C; Ausbeute: 40 bis 50% der Theorie; Hydrochlorid: F. = 82 bis 860C.From 28.5 g (0.1 mol) of β-dimethylaminoethyl (6-methyl-2,5-endomethylene-43-tetrahydrobenzhydryl) ether and 15.6 g (0.1 mol) of ethyl iodide is ß - Dimethylaminoäthyl- (6 @methyl -2,5-endomethylene -43-tetrahydrobenzhydryl) -ether iodoethylate produced. M.p. = 118 to 126 ° C; Yield: 55 to 65% of theory. Example 12 ß-diethylaminoethyl- (6-methyl-2,5-endomethylene-4 3-tetrahydrobenzhydryl) ether From 53.5 g (0.25 mol) of 6-methyl-2,5-endomethylene-4 3-tetrahydrobenzhydrol and 34 g (0.25 mol) of diethylaminoethyl chloride are obtained in in a manner analogous to that in Example 1, the ß-diethylaminoethyl (6-methyl-2,5-endomethylene-43-tetrahydrobenzhydryl) ether. Bp 4 = 136 to 139 ° C; Yield: 40 to 50% of theory; Hydrochloride: m.p. = 82 up to 860C.

Beispiel 3 ß-Piperidinoäthyl-(6-methyl-2,5-endomethylend-tetrahydrobenzhydryl)-äther Aus 53,5 g (0,25 Mol) 6-Methyl-2,5-endomethylen-4 3-tetrahydrobenzhydrol und 37 g (0,25 Mol) Piperidinoäthylchlorid erhält man analog Beispiel l den ß-Piperidinoäthyl- (6 -methyl-2,5 - endomethylen-d 3 - tetrahyd ro -benzhydryl)-äther. Kp.o,$ = 165 bis 169°C; Ausbeute: 45 bis 55 °/o der Theorie; Hydrochlorid: F. = 185 bis 187'C Beispie14 ß-Morpholinoäthyl- (6-methyl-2,5-endomethylen-d 3-tetrahydrobenzhydryl)-äther erhält man aus 53,5 g (0,25 Mol) 6-Methyl-2,5-endomethylen-43-tetrahydrobenzhydrol und 37,5 g (0,25 Mol) Morpholinoäthylchlorid analog Beispiel 1. Kp. 0,4 = 158 bis 162°C; Ausbeute: 25 bis 35 °/o der Theorie; Hydrochlorid: F. = 209 bis212°C Beispiel 5 ß-Pyrrolidinoäthyl- (6-methyl-2,5-endomethylen=43-tetrahydrobenzhydryl)-äther erhält man aus 53,5 g (0,25 Mol) 6-Methyl-2,5-endomethylen-43-tetrahydrobenzhydrol und 33,5 g (0,25 Mol) Pyrrolidinoäthylchlorid analog Beispiel 1. Kp.o,s = 144 bis 147°C; Ausbeute: 40 bis 5% der Theorie; Hydrochlorid: F. = 179 bis 184°C. Beispiel 6 ß - Dimethylaminoäthyl - (2,5 - endomethylen - 4 3 - tetrahydro-a-methylbenzhydryl)-äther erhält man aus 53,5 g (0,25 Mol) 2,5-Endomethylen-43-tetrahydro-a-methylbenzhydrol und 27g (0,25 Mol) Dimethylaminoäthylchlorid analog Beispiel 1. Kp.o,, = 138 bis 142°C; Ausbeute: 20 bis 30 °/o derTheorie; Hydrochlorid: F. =173 bis 174°C, Beispiel? ß - Diäthylaminoäthyl - (2,5 - endomethylen - A3 - tetrahyeo=a=methylbenzhydryl)-äther erhält man aus 53,5 g (0,25 Mol) 2,5-Endomethylen-43-tetrahydro-a-methylbenzhydrol und 34 g (0,25 Mol) Diäthylaminoäthylchlorid analog Beispiel 1. Kp.o,S = 143 bis 148°C; Ausbeute: 30 bis 40 °/o der Theorie; Hydrochlorid: F. = 130 bis 132°C.Example 3 ß-piperidinoethyl (6-methyl-2,5-endomethylend-tetrahydrobenzhydryl) ether From 53.5 g (0.25 mol) of 6-methyl-2,5-endomethylene-4 3-tetrahydrobenzhydrol and 37 g ( 0.25 mol) of piperidinoethyl chloride is obtained analogously to Example 1, the β-piperidinoethyl- (6-methyl-2,5-endomethylene-d 3-tetrahydro-benzhydryl) -ether. Bp $ = 165 to 169 ° C; Yield: 45 to 55% of theory; Hydrochloride: F. = 185 to 187'C Beispie14 ß-Morpholinoäthyl- (6-methyl-2,5-endomethylene-d 3-tetrahydrobenzhydryl) ether is obtained from 53.5 g (0.25 mol) of 6-methyl 2,5-endomethylene-43-tetrahydrobenzhydrol and 37.5 g (0.25 mol) of morpholinoethyl chloride as in Example 1. Bp. 0.4 = 158 to 162 ° C; Yield: 25 to 35% of theory; Hydrochloride: M.p. = 209 to 212 ° C. Example 5 β-Pyrrolidinoethyl (6-methyl-2,5-endomethylene = 43-tetrahydrobenzhydryl) ether is obtained from 53.5 g (0.25 mol) of 6-methyl-2 , 5-endomethylene-43-tetrahydrobenzhydrol and 33.5 g (0.25 mol) of pyrrolidinoethyl chloride analogous to Example 1. Kp.o, s = 144 to 147 ° C; Yield: 40 to 5% of theory; Hydrochloride: m.p. = 179 to 184 ° C. Example 6 β-Dimethylaminoethyl (2,5 -endomethylene-4 3-tetrahydro-α-methylbenzhydryl) ether is obtained from 53.5 g (0.25 mol) of 2,5-endomethylene-43-tetrahydro-α-methylbenzhydrol and 27g (0.25 mol) of dimethylaminoethyl chloride analogous to Example 1. Kp.o ,, = 138 to 142 ° C; Yield: 20 to 30% of theory; Hydrochloride: F. = 173 to 174 ° C, example? ß - Diethylaminoethyl (2,5 - endomethylene - A3 - tetrahyeo = a = methylbenzhydryl) ether is obtained from 53.5 g (0.25 mol) of 2,5-endomethylene-43-tetrahydro-a-methylbenzhydrol and 34 g (0.25 mol) diethylaminoethyl chloride analogous to Example 1. Kp.o, S = 143 to 148 ° C; Yield: 30 to 40% of theory; Hydrochloride: m.p. = 130 to 132 ° C.

Beispiel 8 '- -- ß-Piperidinöäthyl-(2,5-endomethylen-43-tetrahydroa - methyl - benzhydryl) - äther erhält man aus 53,5 g (0;25 Mol) 2,5-Endömethylen-43-tetrahydro-a-methylbenzhydrol und 37 g (0,25 Mol) Piperidinoäthylchlorid analog Beispiel 1. Kp.o,s = 157 bis 165°C; Ausbeute: 30 bis 40 % der Theorie; Hydrochlorid: F.--=* 178 bis 180°C. . _ Beispiel 9 ß-Morpholinoäthyl-(2,5-endomethylen-d 3-tetrahydroa-methylbenzhydryl)-äther erhält man aus 53,5 g (0,25 Mol) 2,5-Endomethylen-d 3-tetrahydro-a-methylbenzhydrol und 37,5 g (0,25 Mol) Morpholinoäthylchlorid analog Beispiel 1. Kp.o,$ = 168 bis 172°C, Ausbeute: 10 bis 20°/a der Theorie; Hydrochlorid: F. = 165 bis 167°C.Example 8 '- - ß-Piperidinöäthyl- (2,5-endomethylene-43-tetrahydroa - methyl - benzhydryl) - ether is obtained from 53.5 g (0.25 mol) of 2,5-endomethylene-43-tetrahydryl a-methylbenzhydrol and 37 g (0.25 mol) of piperidinoethyl chloride analogous to Example 1. Kp.o, s = 157 to 165 ° C; Yield: 30 to 40% of theory; Hydrochloride: F .-- = * 178 to 180 ° C. . Example 9 β-morpholinoethyl (2,5-endomethylene-d 3-tetrahydroa-methylbenzhydryl) ether is obtained from 53.5 g (0.25 mol) of 2,5-endomethylene-d 3-tetrahydro-a-methylbenzhydrol and 37.5 g (0.25 mol) of morpholino ethyl chloride analogous to Example 1. Kp.o, $ = 168 to 172 ° C, yield: 10 to 20 ° / a of theory; Hydrochloride: m.p. = 165 to 167 ° C.

Beispiel 10 ß-Pyrrolidinoäthyl- (2,5-endomethylen-d 3-tetrahydroa-methylbenzhydryl)-äther erhält man aus 53,5 g (0,25 Mol) 2,5-Endomethylen-43-tetrahydro-a-methylbenzhydrol und 33,5 g (0,25 Mol) Pyrrolidinoäthylchlorid analog Beispiel 1. Kp.o" = 153 bis 158°C; Ausbeute: 50 bis 60 °% der Theorie; Hydrochlorid: F. = 165 bis 167°C.Example 10 β-pyrrolidinoethyl (2,5-endomethylene-d 3-tetrahydroa-methylbenzhydryl) ether is obtained from 53.5 g (0.25 mol) of 2,5-endomethylene-43-tetrahydro-a-methylbenzhydrol and 33 , 5 g (0.25 mol) of pyrrolidinoethyl chloride analogous to Example 1. Kp.o "= 153 to 158 ° C; Yield: 50 to 60 °% of theory; hydrochloride: mp = 165 to 167 ° C.

Beispiel 11 ß - Dimethylaminoäthyl- (4' -chlor -2,5 - endomethylen -d 3-tetrahydro-a-methylbenzhydryl) -äther erhält man aus 62 g (0,25 Mol) 4'-Chlor-2,5-endomethylen-43-tetrahydroa-methylbenzhydrol und 27 g (0,25 Mol) Dimethylaminoäthylchlorid analog Beispiel 1. Kp.o,2 = 140 bis 145°C; Ausbeute: 35 bis 45°/o der Theorie; Hydrochlorid: F. _ 162 bis 163°C.Example 11 β-Dimethylaminoethyl- (4'-chloro -2,5-endomethylene -d 3-tetrahydro-α-methylbenzhydryl) ether is obtained from 62 g (0.25 mol) of 4'-chloro-2,5-endomethylene -43-tetrahydroa-methylbenzhydrol and 27 g (0.25 mol) of dimethylaminoethyl chloride analogous to Example 1. Kp.o.2 = 140 to 145 ° C; Yield: 35 to 45% of theory; Hydrochloride: m.p. 162 to 163 ° C.

Das jodmethylat erhält man aus 32 g (0,1 Mol) ß-Dimethylaminoäthyl-(4'-chlor-2,5-endomethylen - 4 3-tetrahydro-a-methylbenzhydryl)-äther und 14,2 g (0,1 Mol) Methyljodid analog Beispiel 2. F. = 177 bis 182°C. Ausbeute: 80 bis 90 % der Theorie.The iodomethylate is obtained from 32 g (0.1 mol) of ß-dimethylaminoethyl (4'-chloro-2,5-endomethylene-4 3-tetrahydro-a-methylbenzhydryl) ether and 14.2 g (0.1 mol ) Methyl iodide analogous to Example 2. F. = 177 to 182 ° C. Yield: 80 to 90 % of theory.

Beispiel 12 ß-Dimethylaminoäthyl- (6-methyl-2,5-endomethylen-43-tetrahydro-a-methylbenzhydryl)-äther erhält man aus 57 g (0,25 Mol) 6-Methyl-2,5-endomethylen-d 3-tetrahydroa-methylbenzhydrol und 27 g (0,25 Mol) Dimethylaminoäthylchlorid analog Beispiel 1. Kp.o,4 = 123 bis 135°C; Ausbeute: 15 bis 25°/o der Theorie; Hydrochlorid: F. _ 169 bis 171'C. Example 12 β-Dimethylaminoethyl (6-methyl-2,5-endomethylene-43-tetrahydro-α-methylbenzhydryl) ether is obtained from 57 g (0.25 mol) of 6-methyl-2,5-endomethylene-d 3 tetrahydroa-methylbenzhydrol and 27 g (0.25 mol) of dimethylaminoethyl chloride analogous to Example 1. Kp.o, 4 = 123 to 135 ° C; Yield: 15 to 25% of theory; Hydrochloride: m.p. 169 to 171 ° C.

Beispiel 13 ß-Dimethylaminoäthyl- (6 -methyl-2,5-endomethylenhexahydro-a-methylbenzhydryl)-äther erhält man aus 57,5 g (0,25 Mol) 6-Methyl-2,5-endornethylenhexahydroa-methylbenzhydrol und 27 g (0,25 Mol) Dimethylaminoäthylchlorid analog Beispiel 1. Kp.o,s = 154 bis 158°C; Ausbeute: 35 bis 45°/o der Theorie; Hydrochlorid: F. _ 197 bis 198°C.Example 13 β-Dimethylaminoethyl- (6-methyl-2,5-endomethylene-hexahydro-α-methylbenzhydryl) -ether is obtained from 57.5 g (0.25 mol) of 6-methyl-2,5-endornethylenhexahydroa-methylbenzhydrol and 27 g (0.25 mol) of dimethylaminoethyl chloride analogous to Example 1. Kp.o, s = 154 to 158 ° C; Yield: 35 to 45% of theory; Hydrochloride: mp 197-198 ° C.

Claims (1)

PATENTANSPRUCH: Verfahren zur Herstellung neuer, spasmolytisch wirksamer, basischer Äther der allgemeinen Formel in der R1 und R, für niedere Alkylreste stehen, die gegebenenfalls zusammen mit dem Stickstoffatom einen heterocyclischen Rest bilden können, R3 für einen 2,5-Endomethylencyclohexyl- oder einen 2,5-Endomethylen-d 3-cyclohexenylrest steht, der gegebenenfalls in 6-Stellung durch einen niederen Alkylrest substituiert sein kann, R4 Wasserstoff oder einen niederen Alkylrest bedeutet, R3 ein 6-Alkyl-2,5-endomethylen-d 3-cyclohexenylrest ist und R4 nur für Alkyl steht, wenn R3 ein 2,5-Endomethylen-43-cyclohexenylrest ist und X Wasserstoff oder Halogen bedeutet, sowie deren Salze mit physiologisch unbedenklichen Säuren, vorzugsweise Chlorwasserstoffsäure, bzw. quaternären Ammoniumverbindungen, dadurch gekennzeichnet, daß ein Carbinol der allgemeinen Formel in der R3, R4 und X die vorerwähnte Bedeutung haben, mit einer Verbindung der allgemeinen Formel in der R1 und R2 die obige Bedeutung haben und Hal für ein Halogenatom, vorzugsweise Chlor, steht, in an sich bekannter Weise kondensiert .wird und die erhaltenen Aminoäther in üblicher Weise in die vorerwähnten Salze bzw. mit Alkylestern in quaternäre Ämmoniumverbindungen übergeführt werden. In Betracht gezogene Druckschriften: Deutsche Patentschrift Nr. 955 895.PATENT CLAIM: Process for the production of new, spasmolytically effective, basic ethers of the general formula in which R1 and R, stand for lower alkyl radicals, which can optionally form a heterocyclic radical together with the nitrogen atom, R3 stands for a 2,5-endomethylenecyclohexyl or a 2,5-endomethylene-d 3-cyclohexenyl radical, which is optionally in 6 -Position can be substituted by a lower alkyl radical, R4 is hydrogen or a lower alkyl radical, R3 is a 6-alkyl-2,5-endomethylene-d 3-cyclohexenyl radical and R4 is only alkyl when R3 is a 2,5-endomethylene -43-cyclohexenyl radical and X is hydrogen or halogen, and salts thereof with physiologically acceptable acids, preferably hydrochloric acid, or quaternary ammonium compounds, characterized in that a carbinol of the general formula in which R3, R4 and X have the aforementioned meaning with a compound of the general formula in which R1 and R2 have the above meaning and Hal stands for a halogen atom, preferably chlorine, is condensed in a manner known per se and the amino ethers obtained are converted in the usual way into the aforementioned salts or with alkyl esters into quaternary ammonium compounds. Documents considered: German Patent No. 955 895.
DEA27439A 1957-06-29 1957-06-29 Process for the production of new, spasmolytically effective, basic ethers, their salts or quaternary ammonium compounds Pending DE1052982B (en)

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DEA27439A DE1052982B (en) 1957-06-29 1957-06-29 Process for the production of new, spasmolytically effective, basic ethers, their salts or quaternary ammonium compounds
CH876163A CH374990A (en) 1957-06-29 1958-06-27 Process for the production of new, spasmolytic compounds
CH6113858A CH371112A (en) 1957-06-29 1958-06-27 Process for the production of new, spasmolytic compounds

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DEA27439A DE1052982B (en) 1957-06-29 1957-06-29 Process for the production of new, spasmolytically effective, basic ethers, their salts or quaternary ammonium compounds

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Cited By (3)

* Cited by examiner, † Cited by third party
Publication number Priority date Publication date Assignee Title
DE1108684B (en) * 1960-01-29 1961-06-15 Boehringer & Soehne Gmbh Process for the production of new basic ethers
DE1126383B (en) 1959-08-06 1962-03-29 Olivier Paul Gaudin Process for the production of locally anesthetically effective amino ethers
DE1152410B (en) * 1959-04-01 1963-08-08 Koninklijke Pharma Fab Nv Process for the preparation of dibenzocycloheptane derivatives with spasmolytic and central effects

Citations (1)

* Cited by examiner, † Cited by third party
Publication number Priority date Publication date Assignee Title
DE955895C (en) * 1953-08-05 1957-01-10 Gross Berliner Eisenmoebel Fab Safety device for the support frame of the headboard of a bed, in particular a hospital bed

Patent Citations (1)

* Cited by examiner, † Cited by third party
Publication number Priority date Publication date Assignee Title
DE955895C (en) * 1953-08-05 1957-01-10 Gross Berliner Eisenmoebel Fab Safety device for the support frame of the headboard of a bed, in particular a hospital bed

Cited By (3)

* Cited by examiner, † Cited by third party
Publication number Priority date Publication date Assignee Title
DE1152410B (en) * 1959-04-01 1963-08-08 Koninklijke Pharma Fab Nv Process for the preparation of dibenzocycloheptane derivatives with spasmolytic and central effects
DE1126383B (en) 1959-08-06 1962-03-29 Olivier Paul Gaudin Process for the production of locally anesthetically effective amino ethers
DE1108684B (en) * 1960-01-29 1961-06-15 Boehringer & Soehne Gmbh Process for the production of new basic ethers

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Publication number Publication date
CH374990A (en) 1964-02-15
CH371112A (en) 1963-08-15

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