DE2854308A1 - ANTICHOLINERGIC SUBSTANCES WITH ANTISECRETORIC EFFECT, THEIR PRODUCTION AND USE - Google Patents

Description

^! 854308

INTERx RESEARCH CORPORATION

Lawrence, Kansas 66o44 V.St.A.

Anticholinergic substances raib antisecretory Effect, their production and use

The invention also relates to certain anticholinergics antisecretory effect, especially "soft" anticholinergic and antisecretory substances that are substantially anticholinergic and antisecretory, respectively act and have only low toxicity in cosmetic and therapeutic use, as well as pharmaceuticals

and cosmetic compositions containing these substances, including their use.

The invention relates to compounds of the formulas

R c - C - X - CH - N ^ - iß (I)

RO-CX-CH -N ^ Y ⁰ (II), R ₄ 0

in which mean:

N ^ a tertiary amine,

an unsaturated arain,

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7S AT 207 BOD ^SI

^{SI / rm}

Rp, R-, and Rjj simultaneously or independently

H, an open chain C.- to Cq-

Alkyl group,
a cycloalkyl or cycloalkenyl

group with up to 8 carbon atoms, a C ₁ - to Cg-alkoxyalkyl group, a C- to Cg-acyloxyalkyl group, a C ..- to Cn-haloalkyl group, a C ^ - to Cg-carboxyalkyl group, a Cp- bis Cg-alkenylphenyl group, an aryl group or by halogen, C ₁ - to C ^ substituted -O-alkyl, O-acyl, nitro, carboxy or carbethoxy aryl group, -CH ₂ -OH, -CH ₂ -OCOR ₁ ^1, wherein R ₁ 'means the same as below R ₁ or -CH ₂ -ONO ₂ ,

-OH, halogen, -OCOR ₁ with R ₁ as below or -ONO ₂ ,

where at least two of the substituents R ₃ , R, and R ₁ ^ are different from hydrogen and R ₂ , R, and R ₁ , together have at least b C atoms or Rp, R, and Rj, together with the ot-c- Atom to which they are attached form a condensed polycarbocyclic or polyheterocyclic ring,

R _{1 the} same as R ₂ , R-. or R _i} ,

X -0- or -S-

and

Y is halogen or an equivalent

organic or inorganic monovalent anion.

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- yar -

The compounds have anticholinergic, antisecretory activity.

Already known anticholinergic and antisecretory Effective agents such as banthines and probanthines are essentially anticholinergic and antisecretory Effectiveness, however, besides these main effects also have numerous toxic side effects, which can be seen through Express the occurrence of dizziness, blurred vision, dry mouth and the like.

According to the invention, on the basis of detailed experimental investigations of analogous conventional compounds, it was found that that all such compounds have a 2-carbon atom bond between the X in formulas (I) and (II) Have substituents and the adjacent nitrogen atom of the amino group.

On the basis of extensive experimental investigations, it was found that when a carbon atom is present existing bridge between the substituent X and the adjacent nitrogen atom of the amino group of the remainder Entire molecule has an essentially anticholinergic and antisecretory activity. Furthermore it was found that the resulting compounds were made up of one carbon atom due to the presence of them Bridge very easily hydrolytically and / or enzymatically

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can be split, resulting in a non-toxic and non-toxic non-anticholinergic effectiveness of the resulting Byproducts. Further investigation also showed that this effect is due to a destruction of the quaternary Center of the entire molecule is based as follows:

R_-CCO-CH-N ^ Y or R ₃ -CCO-CH-N:

R ₄ O

R ₄ O

H ₂ O

R -C-COOH + R ₁ -CHO +
3 ι '

HY + N ^ or

4th
The selected compounds according to the invention have high activity against peripheral receptor sites such as the stomach wall, sweat glands and the like and have essentially no central anticholinergic activity since they are unable to penetrate the blood-brain barrier and are split after their penetration into the general circulation will.

The invention is based on the object of novel anticholinergic to indicate effective substances with a substantial antisecretory effectiveness due to their molecular structure remain practically nontoxic in cosmetic or, in particular, therapeutic use, as well as a method for producing these Substances and their use, in particular in pharmaceutical compositions.

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The object is achieved according to the claim.

In the above formulas, an aryl group is a phenyl or naphthyl group, and a halogen group is a suitable one Halogen such as chlorine, bromine or iodine is understood as meaning 'acyl' in terms such as acyloxyalkyl and O-acyl become suitable carboacyl groups such as Formyl, acetyl, propionyl, benzoyl and the like are understood. The adjective "substituted" means in context with the substituted aryl group that the aryl function can be substituted with one or more of the substituents specified for this purpose. When the substituent Y means no halogen, it preferably represents methanesulphonate, fluorosulphonate or tosylate.

The term "unsaturated amine" means ^ -heterocyclic Unsaturated systems with 3 to 10 ring members and substituted derivatives thereof understood their unsaturation corresponds to the maximum number of non-cumulative double bonds with the prerequisite that the nitrogen atom does not have a hydrogen atom as a substituent. This definition is supplemented by those listed below exemplified groups:

1-methyl-azirine 9 ^H 3

1-methyl-pyrrole

1-methyl-imidazole

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1-methylpyrazole pyridine TqJ

Pyrazine pyridazine (\

CH.

2-methy1-isoindole 3-H-indole OMnolin

Isoquinoline

Phtbalazine Ohinoxaline Quinazoline Phenazine Isothiazole

Pyrimidine

—CH.

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- a »

10-methyl-phenothiazine-

Isoxazole

Furazan

Li

Of the compounds of the invention of the formulas (I) and (Ii) "Certain compounds are preferred, as follows is explained in detail. Of these, the following compounds are particularly preferred:

1. [d, 1-d-Cyclopentylphenylacetoxymethyl] -triethyl-

-ammonium chloride.

2. 1-fd, 1- ol-Cyclopentylphenylacetoxymethyi] -1-methyl- -morpholinium chloride.

3 · 1 - [d, 1- d-Cyclopentylphenylacet o: xymethyl] -1 -methyl- pyrrolidinium chloride.

4 ·. 1-Ld, l-o (- CyclopentylphenylacetoDς7Πιethyl] -3-methyl- -imidazoliurachloride.

5 · 1- [d, l- oL-OyclopentylphenylacetosymethylJ-i .2-cli- -methylpyrrolidinium chloride.

6. 1 - [d, 1- oL-Cyclopentylphenylacetoxymetyl] -quinuclidinium chloride.

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7. 1 - [d, 1- at-Cyclopentylphenylacetoxymethyl] -3-acetoxy- -cMnuclidinium chloride.

8. i- ^ djl-oC-Cyclopentylphenylacetoxynethyl] -3-ethoxycexbonylpyridinium chloride.

9.1 - [d., 1- ol-Cyclopentylphenylacet o ^ methyl] -tri ^ propoxy- ethylammonium chloride.

10. ^/ 10- [d, l-OL-cyclopentylphenylacetate03q5nnethyl] -10-methyl- phenothiazinium chloride.

11. [d, 1-oL-Oyclohexylphenylacetoxymethyl] -triethylammoniumchlorid.

12. 1- [d, l-cjL-CyclohexylphenylacetO3qymethylj -1 -mettiylmorpholinitiinclilorid.

13 · 1 - [d, 1- cL-CyclohexylphenylacetoaqTmetliyl] -1 -methyl- pyrrolidinium chloride.

14. 1 - [a , 1-Oi. -Oyclohexylphenylacetoxymethyl] -3-methyl- -imidazolium chloride.

15. 1- [d, l-oL-Oyclohexylphenylacetoxymethyl] -1.2-dimethyl- pyrrolidinium chloride.

16. 1 - | _d, 1- d-Cyclohexylphenylacetoxymethyi] -chinu- -clidinium chloride.

17 · i-fdjl-ct-Cyclohe ^ lplienylacetoxymethyl] -3-aceto3qy- -quinuclidinium chloride.

18. i-fdjl-oL-Cyclohexylphenylacetoxymethylj -3-Ä.thoxy- carbonylpyridinium chloride.

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19. i-fdjl-dL-Cyclohexylphenylacetoxymethylj -triLpropoxy- ethylammonium chloride.

20. 10- [d, l-oL-Cyclohexylphenylacetoxyniethyl] -10-methyl- -phenothiazinium chloride.

21. [d, l-2-phenylbutyrylo: xymethyl] -triethylammonium- -chloride.

22. 1 - [d, 1-2-Phenylbutyryloxymethyl] -1 -methylniorplioliiiiuni- -chloride.

23. 1- [d, 1-2-phenylbutyryloxymethyl] -1-methylpyrrolidinium- -chloride.

24. 1- [d, l-2-phenylbutyryloxymethyl] -3-methylimidazolium- -chloride.

25. 1- [d, l-2-phenylbutyrylosyaiethyl] -1.2-dimethyl- pyrrolidinium chloride.

26. 1- [d, 1-2-phenylbutyryloxymethyl] -quinuclidinium- -chloride.

27 «1- £ d j 1-2-phenylbutyryloxymethylJ -3-acetoxychin- -clidinium chloride.

28 _e 1 - [d 51-2-Ph.enylbutyryloxymethyl] -3-ethoxycarbonyl-pyridinium chloride.

29.1 - [d, X-2-PhenylbutyrylO3iyme thylj -tri-propoxyethyl- -ammoniumcb-lorid.

30 "10-f d, l-2-phenylbutyryl03q7methyl] -1O-.methylph.eno- -thiazinium chloride.

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31. [d, 1-2-Methylbutyryloxymethyl] -triethylammonium chloride.

32.1 - [d, 1-2-methylbutyryloxymethyl] -1 -methylmorpholinium- -chloride.

33. 1 - [d, 1-2-methylbutyryloxymethyl] -1 -methylpyrrolidinium- -chloride.

34. 1- [d, l-2-methylbutyrylo3q7metliyl] -3-methylimidazolium- -chloride.

35. Ί - [d, 1-2-methylbutyryloxymethyl] -1.2-dimethyl- pyrrolidinium chloride.

- 1 - [d, 1-2-methylbutyiyloxymethyl] -quinuclidinium- -chloride.

· 1 - [d, 1-2-methylbutyryloxymethyl] -3-acetoxychin- -clidinium chloride.

38.1 - [d, 1-2-methylbutyryloxymethyl] -3-ethoxycarbonyl- pyridinium chloride.

39. 1 - [d, 1-2-methylbutyryloxymethyl] -tr ^ propoxyethyl- -ammonium chloride.

40.10- [d, 1-2-methylbutyryloxymethyl] -10-methylph.eno- -thiaz inium chloride.

41. [Tricyclo (3.3 »1-1) decane-1-carboxymethyl] -triethyl- -ammonium chloride.

42. 1- [Tricyclo (3.3.1.1 ^ '^) decaii-1-carboxymethyl] -1- -methylmorpholinium chloride.

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4-3. 'l- [

Methyl pyrrolidine rum chloride.

44. 1-

-metbylimidazolite chloride.

4-5. 1 - ["Tricyclo (3.3.1.i5 '^) decane-1-carboxymethyl] -1.2-di -methylpyrrolidirLiumchlorid.

46. 1- [a} ricyclo (3.3.1.1 ^ ^#l ' ⁷ ) decaa-'1-carbo3q5nnethyl] -quinuclidinium chloride.

4-7. 1- [Tricyclo (3.5.1.i5-7) d _ecan _-i_ _car -b _OX y _me t] iyi] -3-acet -oxyquinuclidinium chloride.

46. 1- [Tricyclo (3.3. ^/ L. ^/ L ⁵ ' ⁷ ) decane-1-carbo3q5rmethyl] -3- -ethoxycarbonylpyridinium chloride.

4-9. 1 - [! Rricyclo (3.3.1. ^/ 15 '^) decane-1-carboxymethyl] -tri- -propoxyethylammonium chloride.

50. 10
-methylphenothiazini-umclilorid.

51. [d- oL-Oycloliex-S-enylpheiiylacetoxyme-bilylJ -triethylammonium chloride.

52.1 - [d- oL-Oyclohex-2-enylphenylacetoxymethyl] -1-methyl -morpholinium chloride.

· 1 - [d- d. -Oycloh.ex-2-enylpherLyl acetoxymethylj -1 -methyl pyrrolidinium chloride.

54 ·. 1 - [d-cL-cyclohex-2-enylphenylacetoxymethyl] -3-methyl -imidazolium chloride.

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55.1 - [d- dL-Cyclohex-2-enylplienylacetoxymethyl] -1.2-di- methylpyrrolidinium chloride.

56.1 - [d- oL -Gyclohex ^ -enylpkenylacetoxymethyl] -chinu- -clidinium chloride.

57 · 1 - [d- oi- -Gyclohex-2-enylphenylacetoxymethylJ -3-acetoxy- -quinuclidinium chloride.

58. 1- [d-oL-0yclohex-2-enylph.enylacetoxymethyl] -3-ethoxy- carbonylpyridinium chloride.

59 · 1 - [d- cL-Oyclohex-2-enylphenylacetoxymethylJ -tri- -propoxyethylammonium chloride.

60.10- [d-oL-0yclohex-2-enylph.enylacetoxymethyl] -10- -methylphenothiazine chloride.

61. [l- oL-Cyclopropylphenylacetoxymethyl] -triethyl- -ammonium chloride.

62.1 - [1- c ^ -Cyclopropylphenylacetoxymethyl] -1 -methyl- -morpholinium chloride.

63. 1- [l- oL -Oyclopropylphenylacetoxymethyl] -1-methyl- -pyrrolidinium chloride.

64.1 - JjL- cL-Oyclopropylphenylacetoxymethyl] -3-methyl- -imidazolium chloride.

65. I-Ll-OL-Oyclopropylphenylacetoxymethylj -1,2-dimethyl- pyrrolidinium chloride.

66.1 - JjL- oL -Oyclopropylphenylacetoxymethyl] -chinu- -clidinium chloride.

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67. 1- [l-dL - Cyclopropylphenylacetoxyniet; hyl) -3-acetoxy- - quinuclidinium chloride.

68. 1- [1- <± -Cyclopropylphenylacetoxyinethyl] -I-ethoxy- carbonylpyridium chloride.

69. 1- [l- ri ^ -CyclopropylphenylacetoxymethylJ -tri_.propoxy- -ätnyl ammoniumchl ο r i d.

70.10- [l- oi -Oyclopropylphenylacetoxymethyl] -10-methyl- -phenothiazinium chloride.

The compounds of the invention can favorably can be prepared by processes known per se, for example those described in US Pat. No. 3,998,815 Procedures.

A particularly favorable process for the preparation of the compounds according to the invention is accordingly based on the fact that a compound of the general formula III

R _n 0 R,
12 II, 1

R ₃ -CCX-CH- Hai (III)

with R ₁ , Rp, R ^, Rh and X as above and Hai = halogen

with a tertiary amine (N ~) or a unsaturated amine (N ^) is converted,

The reactants are generally used in approximately equimolar proportions; the reaction is carried out in the presence of an inert solvent such as ether, acetonitrile, CH ₂ Cl ₂ and the like at a temperature between room temperature and the reflux temperature of the solvent

909825/0374

solvent carried out for 2 to 2k h.

Alternatively, the reaction can also be carried out in the absence of a solvent by mixing the two reactants together and maintaining a reaction temperature of room temperature or between 20 and 70 ^° C. for 2 to 2 k h.

In both cases, the crystalline salt obtained by recrystallization from ether-ethanol mixtures and the like. getting cleaned.

The starting materials of the formula III, in which X is oxygen, can be obtained by reacting the corresponding aldehyde R ₁

HC = O

with the corresponding acid halide of the formula

R, - C - C - Hai 3 ι Il

R ₄ 0

with R ^, Rp, R ,, R ₁ , and Hai as above.

The starting materials of formula III in which X is sulfur means are by reaction of the aldehyde

?1

HC = O

with a compound of the formula

R, - C - C - SH 3 l ii

R ₁ . 0

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about the intermediate

R ₉ 0 R ₁ CCS-CH-

R ₇ JCCS-CH-OH 3 ι

accessible, which are then reacted with a phosphorus pentahalide to form the desired starting material of the formula III can.

Another route to the starting materials of formula III is based on a compound of the formula

R "0 1 ² H

R ₃ -CCXM

with Rp, R, and R ^ as above,

in which M is an ion of a suitable metal such as Na, K or Tl,

with a compound of the formula

Hai - CH - Hai

R ₁ ^x with R ^ and shark as above

is implemented, in which the two halogen atoms can be the same or different. When the two halogen atoms are the same a large excess of the corresponding dihalo compound is used.

An alternative process for the preparation of the compounds of the formulas I and II in which X is oxygen is based on the reaction of a tertiary amine (N ~) or an unsaturated amine (N ^) with an acyl halide of the formula

- 28a 009825/087 *

R ₀ O
R ₃ -CC-Hal

with Rp, R ,, Rj, and Hal as above

and subsequent reaction of the reaction mixture with an aldehyde of the formula

HC = O

with R ₁ as above,

The amine and the acyl halide are generally used in equimolar amounts, the mixture being kept at room temperature for 2 to 24 hours; then an equimolar amount of the aldehyde is added and the mixture is ^{stirred at room temperature or elevated temperature (up to 75 °} C.) for 2 to 48 hours.

Another process for the preparation of certain selected compounds according to the invention is based on Quaternization of a compound of the formula IV

h 9? i "

R ₃ -CCX-CH-Nd (IV)

with R ₁ , R ₂ , R ₃ , R ^ and X as above,

where N <^ the remainder of any secondary amine means.

This process is of particular interest because of the alkylation of a secondary amine in which a Alkyl halide with the secondary amine indicated above in a suitable solvent such as acetonitrile or about nitromethane is implemented.

- 28b 609825/0874

The starting materials of the formula IV can in turn by reacting a compound of the formula

R ₀ O
R, -CCXM

^R 4

with R ₂ , R ,, R ₁ ^ and X as above,

in which M is an alkali or alkaline earth metal or another suitable metal, for example Well, K, Tl, means

with a compound of the formula V.

HaI-CH-NC (V)

with R. as above,

in which N <means the remainder of a secondary amine,

in a suitable solvent such as dichloromethane or Tetrahydrofuran can be produced.

The compounds of the formula V can, for example, by reacting 2 mol of any secondary amine of a dialkylamine Sj of a cycloalphatic amine such as Morpholine piperidine or piperazine or an unsaturated one Amine j in which the unsaturated bond is not adjacent to the nitrogen atom, for example imidazole, with an aldehyde of the formula

HP-O

with R ₁ as above

under basic reaction conditions and subsequent reaction of the resulting compound of the formula

^ N-CH- N <
with a benzoyl halide in ether or tetrahydrofuran

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can be prepared, whereupon the desired compound of formula V is obtained.

If, on the other hand, compounds according to the invention are sought in which Y is not halogen, for example the 5-sulfosalicylates or compounds in which Y is -R ₂ SO-, where R _{2 is} C ₁ - to C ₂₀ alkyl, for example methanesulfonates, or Y Phenyl, substituted phenyl, in particular alkyl-substituted phenyl such as corresponding p-toluenesulfonates or naphthylj, can use the procedures given above for the preparation of the compounds of the formulas I and II

can be used in which Y is halogen, whereupon the counterion is exchanged.

The exchange of the counterion in the quaternary ammonium salt can take place, for example, with an anion exchange resin. In this procedure, the quaternary ammonium salt is first converted into its OH form and then neutralized with the conjugate acid of the desired base. It was found, however, that in some Cases a different and generally more favorable procedure for exchanging the counterion in the quaternary ammonium salts can be applied, which proceeds schematically as follows!

R-I / T \

? 2 Fl Φ R ^ -CCX-CH-N

3iii R ₁₁ O

R ₀

I 2 ι χ w

and R ^ -C-C-X-CH-N ^, respectively

θ 3 ι μ \

1 R ₄ O γ.

HY

CH, OH

R4O

respectively.

fl

CH

■ B

CH ₃ Y ₁ + H ₂ O,

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- 28d -

- * 8ö -

where Y ₁ J, Br or Cl

mean.

Br, Cl, -CH ₃ SO ,, -CgH ₅ SC re suitable acid ions

or other-

According to the above scheme, a methanolic solution of the acid HY ₂ with the quaternary ammonium halide to form the corresponding methyl halide as well
of the corresponding quaternary ammonium salt · Y- reacted.

This procedure is in the publication of
JJ Kaminski, KW Knudsen and NS Bodor ¹ A Convenient Method for an Ion Exchange in Quaternary Salts ¹ , Tetrahedron VoI 34 (1978) pp 28-57.

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The invention is explained in more detail below with reference to exemplary embodiments, the details of which are not restrictive are.

Example 1 explains the production of starting materials under 1. to 7. and 10. to 11.; the steps 8. and 9 · relate to the explanation of the procedure for the preparation of compounds according to the invention.

The remaining examples all relate to compounds according to the invention.

example 1 Manufacture of 'soft' alkylating agents

The following 'soft ^1. Alkylating agent a catalytic amount of ZnCl ₂ of both components were prepared from the corresponding acyl halides and paraformaldehyde by heating an equimolar mixtures to 90 to 100 ⁰ C in the presence prepared. The raw products were purified and characterized as follows:

1. Chloromethyl-d, 1- oi-cgrclopentylphenylaeetat :

The crude product was transferred to Florisil (0.074 to 0.150 mm,

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100 to 200 mesh) (chloroform) chromatographed; IR spectrum (pure): 2920, 2840, 1750, 1450, 1315, 1110, 1025, 760 and 700 cm "¹; PHR (CDGl ₅ ): 4 7.3 (s, 5H), 5.7 to 5, 2 (m, 2H), 3.3 (d, 1H) and 3.0-0.8 (bm, 9H) ppm.

2. Chloromethyl-d, 1- Ql-cyclohexylphenyl acetate :

The crude product was chromatographed on Florisil (0.074-0.150 mm, 100-200 mesh) (chloroform) and dried in vacuo to a white solid; F. 53 "to 54 ⁰ C; IP Spectrum (KBr): 2910, 2840, 1740, 1490, 1435, 1350, 1280, 125O, 1215, 1130, 1100, 1020, 1000, 770, 730, 710 and 690 cm "¹; PMR (CDCl,): 6 7.3 (s, 5H), 5.7 to 5.5 (m, 2H), 3.3 (d, 1H) and 2.4 to 0.5 (bm, 11H) ppm.

Analysis results: calculated for C ^ cH ^ qo

C: 67.54 ⁰ M H: 7.18%. found: C: 67.40 % \ H: 7.22 %.

3. Chloromethylphenyl acetate :

The crude product was chromatographed on Florisil (0.074-0.150 mm, 100-200 mesh) (chloroform) to give a colorless liquid; Bp 132 to 134 ⁰ C / 14 Torr (Literature: Kp I38 to I5O ⁰ C; B.% 435th). IR spectrum (pure): 3040, 1760, 150, 1455, 1440, 1350, 1260, 1235, 1125, 1030 and 720 cm "¹; PMR (CDCl ₃ ): 6 7.3 (s, 5H), 5, 6 (s, 2H) and 3.6 (s, 2H) ppm.

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4. Chloromethyl-d, 1-2-phenylbutyrate :

The crude product was chromatographed on Florisil (0.074-0.150 mm, 100-200 mesh) (chloroform) to give a colorless liquid; Bp. 103 "to 105 ⁰ C / / 1.8 Torr; IR spectrum (pure): 2970, 1750, 1490, 1450,

1260, 1210, 1195, 1140, 1110, 1075, 1040, 1020, 740, 720 and 700 cm "¹; PMR (CDCl ₃ ): 4 7.2 (s, 5H), 5.5 (s, 2H), 3.4 (t, 1H), 2.5 to 1.4 (m, 2H) and 0.9 (t, 3H) ppm.

5. chloromethyl-d, 1-2-methylbutyrate ;

The crude product was distilled, whereupon a colorless liquid was obtained; Bp 34 to 37 ° C / 1 torr; IR spectrum (pure): 2950, 2930, 2870, 1750, 1450, 1110, 1070, 1030 and 710 cm "¹; PMR (pure): <J 5.7 (s, 2H), 2.7 to 2, 1 (m, 1H), 2.0 to 1.3 (m, 2H), 1.2 (d, 3H) and 0.9 (t, 3H) ppm.

6. Chlorinethyl-d, 1-2-phenylpropionate :

The crude product was chromatographed on Plorisil (0.074-0.150 mm, 100-200 mesh) (chloroform) to obtain a colorless liquid; Bp 101-105 ° C / 1.9 mm; IR spectrum (pure): 3Ο5Ο, 3020, 2970, 293Ο, I75O, 1490, 1450, 1140, 1100, 1080, 720 and 700 cm "¹; PMR (CDCl ₃ ): A 7.2 (s, 5H), 5.6 (s, 2H), 3.8 (q, 1H) and 1.5 (d, 3H) ppm.

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7 · chloromethyl-tricyclo Γ3 »3> 1» 1 J decane-1-carbo: xylate ;

The crude product was chromatographed on Florisil (0.074-0.150 mm, 100-200 mesh) (chloroform) to give a colorless liquid; IR spectrum (neat): 2910, 2860, 1750, 14-50, 1215, Ή85, 1065, 750 and 710 cm "¹; PMR (ODOL ₅ ): j 5.7 (s, 2H) and 2.2 bis 1.6 (m, I5H) ppm.

Analysis results: calculated for C ,, CH ^ qCIN ₂ O ₂ :

0: 61.12%; H: 6.50%; N: 9.50 %. found: C: 60.94%; H: 6.76%; N: 9.37%.

8. Phenylacetate 03gymethyl-1-methylmorpholinium chloride :

A mixture of 1-methylmorpholine (1.8 ml, 0.016 mol) and chloromethylphenyl acetate (3.0 g, 0.016 mol) in anhydrous chloroform (25 ml) was heated ^{to 80 ° C. overnight.} A white precipitate was collected, which was recrystallized from an ethanol-ether mixture, whereupon phenylacetoxymethyl-1-methylmorpholinium chloride was obtained; F. 184 to I85 ⁰ C (0.9 g, 0.003 mol, yield 20%); iR spectrum (KBr); 1735, 1430, 1340, 1320, 1210, 1135, 1095, 1070, 1050, 990, 920, 860, 740 and 710 cm "¹; PMR (D ₂ O): <} 7.4 (s, 5H), 5 , 4 (s, 1H), 4.2 to 3.8 (m, 7H), 3.5 to 3.3 (m, 4H) and 3.2 (s, 2H) ppm.

9. d. 1-3- (1-methylpyrrolidinium) phthalid bromide ;

A mixture of 1-methylpyrrolidine (0.73 ml, 0.007 mol)

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and 3-bromophthalide (1.5 g, 0.007 mol) was heated to 90 ° 0 for 30 min. After cooling to room temperature, the resulting solid was triturated with dry ether, filtered and recrystallized from an ethanol-ether mixture. The product was dried in vacuo to give a white solid; M.p. 162 to 165 ⁰ (1.6 g, 0.005 mol, yield 76%); IR spectrum (KBr): 1790 cm "¹; PMR (D ₂ O): J 8.1 (m, 4H), 6.9 (s, 1H), 4.3 to 3.7 (m, 4- H), 2.9 (s, 3H) and 2.6 to 2.2 (m, 4H) ppm.

Analysis results: calculated for C, j, H ^ ₂

G: 52.37 ⁰ M H: 5.41%; N: 4.70 %. found: C: 52.38%; H: 5.40%; N: 4.93 %>

10. Chloromethyl thioacetate :

(1) Manufacture of hydroxymethylacetyl sulfide :

21.97 B (0.29 mol) thioacetic acid were _{freed from oxygen with an N 2} -StIOm for 15 min. Subsequently, were added paraformaldehyde, and the mixture stirred 3 and was heated to 97 ⁰ O 8.7 g (0.29 mol). Thereafter, the entire amount of paraformaldehyde had gone into solution, whereupon the product was isolated by distillation. B.p. 60 ° 0/10 torr; Yield: 12.17 g, corresponding to 47 d. Th .; Nuclear Magnetic Resonance Spectrum: ^ 4.1 (HO-C, singlet) and ^ 5.1 (S-CH ₂ -O, singlet).

(2) Production of chloromethylthioacetate :

To an ice-cooled solution of 24.3 g

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(0.12 mol) PCIc in 250 ml of anhydrous ethyl ether were added under F ₂ and stirring, 12.17 g (0.12 mol) of hydroxymethylacetyl sulfide so slowly that the reaction temperature ^{did not rise above 13 ° C.} The reaction mixture was then allowed to warm to room temperature over 30 minutes. The ether was then evaporated, whereupon the residue was vacuum distilled _{from POCl 5} and CH ₅ CSCH _{2 Cl.} POCl ₅ distilled at 35 ° C / 15 torr, the product at 32 ° C / 3 torr. The yield was 4.81 g, corresponding to 34 % of theory . Th. NMR spectrum: 6 2.4 (H ₅ C =O, singlet); ^ 4.95 (ClCH ₂ S, singlet).

11. chloromethylphenyl-oL-methylthioacetate ;

The compound was prepared from the corresponding thioacid according to process step (10) above.

Example 2

d, 1- o l-Cyclopentylphenylacetoixymethyltriethylammonium- chloride s

First, chloroform was distilled before use Made anhydrous via phosphorus pentoxide. Then triethylamine (2.5 ml, 0.018 mol) became a stirred solution of chloromethyl-d, 1-p-cyclopentylphenyl- acetate (4.8 g, 0.019 mol) in anhydrous chloroform (5 oil) added. The reaction vessel was then sealed, placed in an oil bath and left on overnight

8098 2 5/0874

75 ⁰ O held. After cooling to room temperature, anhydrous ether was added, whereupon the reaction product was triturated with ether until crystallization began. The deposited solid was separated by filtration under a nitrogen atmosphere and washed thoroughly with anhydrous ether. After drying the product over calcium sulfate in vacuo at 50 ^° C., a white, hygroscopic solid was obtained; M.p. 14-7 "to 14-8 ° 0 (5.3 Si 0.015 mol, yield 83%); IR spectrum (KBr): 1740 cm"¹; PMR (CDCl ₃ ): { 7.3 (s, 5H), 5.6 (s, 2H) and 3.6-0.8 (m, 25H) ppm.

Analysis results: calculated for

C: 67.87%; H: 9.11%; N: 3.96 #. found: C: 67.63%; H: 9.24%; N: 3.95%.

Using the procedure described in Example 2 the following alkylcarboxymethylammonium salts were synthesized:

Example 3

d, 1- cL ^ Cyclopentylphenylacetoxymethyl-i-methylmorpholinium- chloride :

M.p. 166 to 168 ^° C; PMR (CDCl ₃ ): ^ 7.4- (s, 5H), 5.8 (bs, 2H) and 4x, 4- to 0.6 (m, 21H) ppm.

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Example 4

d, 1-oil -Cyclohexylph.enylacetoxymetbyltriäthylammoiiitun- chloride ;

M.p. 128 "to 129 ⁰ C; IR spectrum (KBr): 1740 cm"¹; PMR (CDCl ₅ ): i 7.3 (s, 5H), 5.6 (s, 2H), 3.6 to 3.0 (m, and 2.7 "to 0.7 (m, 20H) ppm .

Analysis results: calculated for Cp ^ H ^ p

C: 68.55%; H: 9.31%; N: 3.81 %. found: C: 68.31%; H: 9.54%; N: 3.71 %.

Example 5

d, 1- oL-Cyclopentylphenylacetoatymethyl-i -methyl- -pyrrolidinium chloride:

M.p. 144 to 145 ^° C; iR 'spectrum (KBr): 1740 cm ""¹; PMR (CDCl ₃ ): h 7.3 (s, 5H), 5.7 (s, 2H) and 4.0-0.7 (m, 21H) ppm.

Analysis results: calculated for C

C: 67.54%; H: 8.35 % \ N: 4.14 %. found: C: 67.76 % \ H: 8.60%; N: 4.02 %.

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Example 6 Tricyclo (3.3.1 « ^{/ 10}

pyrrolidinium chloride:

M.p. 181 to 182 ^° C; IR spectrum (EBr): 1730 cm "¹; PMR (CDCl ₃ ): <i 5.7 (s, 2H), 4.1 to 3.7 (m, 4H), 3.5 (s, 2, 6 to 2.2 (m, 4H) and 2.2 to 1.6 (m, I5H) ppm.

Analysis results: calculated for C

C: 65.06%; H: 8.99 ⁰ M N: 4.46%. found: C: 64.95 H M ^0: 9, 06%; Ή: 4.27%.

Example 7

1- (Tricyclo [3.3 * 1.1 J decane-1-carbO3cymet33 _t yl) -3-meth, yl · imidazolium chloride :

M.p. 158 to 164 ^° C; IR spectrum (KBr) ι 1730 cm ^"1; PMR (CDCl _5): 10.6 ^ (m, 1H), 8.0 (m, 1H), 7.6 (m, 1H), 6.3 ( s, 2H), 4.2 (s, 3H) and 2.2 to 1.6 (m, I5H) ppm.

Analysis results: calculated for C _x ,, JL

C: 61.83%; H: 7.46%; N: 9.01%. found: C: 62.09 ⁰ M H: 7.76%; IT: 8.80%.

Example 8

1 - (d, 1-2-Phenylbutyryloxymetnyl) -3-methylimidazolium- chloride:

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M.p. 89 "to 94 ⁰ C; IR spectrum (KBr): 1740 cm"¹; PMR (CDCl ₃ ): <£ 10.5 (m, 1H), 8.0 (m, 1H), 7.5 (m, 1H), 7.2 (s, 5H), 6.3 (s, 2H), 4.1 (s, 3H), 3.5 (t, 1H), 2.0 (m, 2H) and 0.9 (t, 3H) ppm.

Example 9

Phenylacetoxymethyl-I-metallaylmorpholinium chloride :

A mixture of 1-methylmorpholine (1.8 ml, 0.016 mol) and chloromethylphenyl acetate (3.0 g, 0.016 mol) in anhydrous chloroform (25 ml) was heated ^{to 80 ° C. overnight.} Thereafter, a white precipitate was collected, which was recrystallized from an ethanol-ether mixture, after which phenylacetoxymethyl-1-methylmorpholinium chloride was obtained. M.p. 184 to 185 ^° C. (0.9 g, 0.003 mol, yield 20%); IR spectrum (KBr): 1735, 1430, 1340, 1320, 1210, 1135, 1095, 1070, IO50, 990, 920, 860, 740 and 710 cm "¹; PMR (D ₂ O): 4 7.4 ( 3, 5H), 5.4 (s, 2H), 4.2 to 3.8 (m, TH), 3.5 to 3.3 (m, 4H) and 3.2 (s, 2H) ppm.

Example 10

d »l-3- (1-methylpyrrolidinium) phthalide bromide:

A mixture of 1-methylpyrrolidine (0.73 ml, 0.007 mol) and 3-bromophthalide (1.5 g, 0.007 mol) was heated for 30 min at 90 ⁰ C. After cooling to room temperature, the resulting solid was triturated with dry ether, filtered off and recrystallized from an ethanol-ether mixture. After drying the product in vacuo, a

S0982 5/0874

white solid obtained; M.p. 162 to 165 ⁰ g (1.6 g, 0.005 mol, yield 76%); IR spectrum (EBr): 1790 cm "¹; PMR (D ₂ O): i 8.1 (m, 4H), 6.9 (s, 1H), 4.3 to 3.7 (m, 4H) , 2.9 (s, 3H) and 2.6 to 2.2 (m, 4H) ppm.

Analysis results: calculated for C ^, H. , -BrNO ₂ :

C: 52.37 % \ H: 5.4-1%; IT: 4.70 % . Found: C: 52.38%; H: 5.40 #; N: 4.93 %.

Example 11

d, l-2-methylbutyrylo3q7meth.yl-1-methylpyrrolidinium chloride :

A mixture of chloromethyl-d, l-2-methylbutanoate (3.02 g, 0.02 mol) and 1-methylpyrrolidine was ^{heated to 90 °} C. for 2 h. After cooling to room temperature, the resulting oil was washed with ether. The ether was then decanted off, after which the product was triturated with ether to initiate crystallization. The d, l-2-methylbutanoyloxymethyl-1-methylpyrrolidinium chloride was isolated as a hygroscopic, white solid; F. 76 to 78 ⁰ C (2.5 g, 0.01 mol, yield 53%); IR spectrum (KBr): 1750 cm "¹; PMR (CDCl ₃ ): & 5.8 (s, 2H), 4.2 to 3.8 (m, 4H), 3.5 (s, 3H), 2.8 to 2.1 (m, 5H), 2.0 to 1.4 (m, 1H), 1.2 (d, 3H) and 1.0 (t, 3H) ppm.

Analysis results: calculated for C _{1 XjH 222}

C: 56.04%; H: 9.41%; N: 5.94 %. found: C: 56.18%; H: 9.53 % \ N: 5.86%.

909825/0874

-Aces

Example 12

d, l-2-methylbutyrylo: kymethyl-1,2-dimethylpyrrolidinium chloride :

The compound was prepared by the same procedure as d, 1-2-methylbutyryloxymethyl-i-methylpyrrolidinium chloride and isolated as a mixture of diastereomers (about 40:60); F. 76 to 78 ⁰ O; IR spectrum (KBr): 1750 cm ""¹; PMR (CDCl ₃ ): a) 6 5.8 (s, 2H), 4.8 to 3.9 (m, 3H), 3.1 (s, 3H), 2.8 to 2.0 (m, 5H), 1.5 Cd, 3H), 1.2 (d, 3H) and 0.9 (t, 3H) ppm; b) «Ä 5.5 (s, 2H), 4.8 to 3.9 (m, 3H), 3.5 (s, 3H), 2.8 to 2.0 (m, 5H), 1, 6 (d, 3H), 1.2 (d, and 0.9 (t, 3H) ppm.

Analysis results: calculated for C, ^ H / -

C: 57.70 ⁰ M H: 9.69% \ N: 5.61%. found: C: 57.56 % \ H: 9.87%; F: 5.79%.

Example 13

d _t l ^ -Methylbutyryloxymethylquinuclidinium chloride :

Chloromethyl d, l-2-methylbutanoate (1.5 g, 0.01 mol) and quinuclidine (1.1 g, 0.01 mol) were mixed together and stirred at room temperature for 24 hours. The resulting oil was triturated with ether to give a white, hygroscopic solid; M.p. 134 to 137 ⁰ O (2.0 g, 0.008 mol, yield 77%); PMR (CDClj): <S 5.6 (s, 2H), 3.0 (bt, 6H), 3.3 (bt, 1H), 2.8 to 1.8 (m, 7H), 1.8 up to 1.3 (m, 2H), 1.2 (d, 3H) and 0.9 (t, 3H) ppm.

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- 4M--

Analysis results : calculated for C ^ -H ₂ ^ ₂

C: 59.64%; H: 9.24%; E: 5.33%. found: C: 59.50 % \ H: 9.48 %; N: 5.09 %.

Example 14

d, l ~ 2 ~ methylbutyryloyymethyl-3-acetoxyquinuclidinium- · chloride ;

The compound was prepared by the same procedure as d, 1-4 -methylbutyryloxymethylquinuclidinium chloride. Mp 130-133 ° C; IR spectrum (KBr): 1730 cm "* ¹ ; PMR (CDOL ₅ ): j 5.8 (s, 2H), 5.4 to 5.1 (m, 1H), 4.8 to 3.4 ( m, 7H), 2.8 to 2.0 (m, 8H), 2.0 to 1.4 (m, 2H), 1.2 (d, 3 * 0 and 0.9 (t, 3H) ppm .

• Analysis ^results: calculated for C., -HpgClNOh:

G: 56.33 ⁰ M H: 8.19% \ N: 4.38%. found: C: 56.10%; H: 8.30%; K: 4.08%.

Examples 15- ^ 0:

Using the procedure described above as well Suitable generally and / or specifically described reactants and process conditions were the following Get connections:

To the formulas

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and

ι , _ G - σ - χ - CH - H =

3 I Il

\ ο

(H)

Example

or

X Y "

16 H.

17 H.

18 H.

19 H.

20 H.

LJ) H Γ T-T 0 Cl or
Br ό
A. H
H ^? " ³ C H ₃ °
H ₃ ° Cl or
Br
Cl or
Br A. H V
CH ₃ O Cl or
Br A. H 0 O Cl or
Br A. H . CH ₃
N
Q O Cl or
Br 9098 2 5 / 0874

S *

For example, play ^K 1 ^Ά 2 or

X Y '

21 CH, [O

H ν-i-Pr 0 Cl or \ _ Br

22 H.

[O;

Cr ¹

CH.

O Cl or

Br

23 H.

CH,

OCH-. CF-, I ^J o
3 ν, .CH ₃

Cl or

Br

24 HOURS

OCH ₃ CF ₃

Cl or

Br

H,

25 H.

C C

ι ι

H H

or

Br

26 H.

C-

NN-CH ₃ O

C] or

Br

27 H.

CH.

^cl or

Br

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example

JSz

or

X X "

28 H.

L- /

_cl Br

[O] CH

o cioder

Br

30 CH

CH.

Cl or Br

31 H.

ch ₃ oc <:

Cl or

Br

32 H.

^H ^ - 'COOC ₂ H ₅

Cl or Br

33 H.

/ ^C 2 ^H 5
NC ₂ H ₅

^C 2 ^H 5

Cl or Br

34 H.

el or

Br

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Co

Z854308

At- τ,
game ¹ H

R-. or

X X "

35 H.

/ ^C 2 ^H 5 NC ₀ H ₁ .

Cl or

Br

36 H.

/ ^C 2 ^H 5

NC ₀ H ₁ .

_N 2 5 C ₂ H ₅

el or

Br

³⁷ CoD approx

C ₀ H- / 25

NC ₂ H ₅ CH

Cloder

Br

38 H (Q

CH,

I.

CH.

CH.

el or Br

39 H.

H CH

NC ₂ H ₅ C ₂ H ₅

Cl or

Br

40 CH ₃ -HC

, CH ₃

VXX ₃

CH-

I ²

CH

CH CH.

Cl or

Br

Θ09825 / 0874

The substituents mentioned in the columns for P1 and R3 represent the entire grouping

R, --C - of formulas I and II; in order to

ο is the case that R, R and R ₁ , together with the

^ -C atom to which they are bound, a condensed polycarboeyclic ring form.

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- 0 * 5 -

Example 4-1 Pharmacological studies

O) in vivo experiments to determine; an anticholinerpic efficacy

Adult cats were anesthetized by intraperitoneal injection of a mixture of OL-chloralose (80 mg / kg) and sodium pentobarbitone (6 mg / kg). The animals were then vagotomized bilaterally and artificially ventilated during the experiments. Arterial blood pressure was recorded on a cannulated carotid artery using a Sta.tham PD23 pressure transducer connected to a Grass ? G inkwriting polygraph. The heart rate was measured routinely using either the arterial pulse or the lead II of the EKG to trigger a cardiotachometer (Grass 7P4-). In all experiments, the substances were injected intravenously into a cannulated arm vein.

The control results were initially determined for a range of different acetylcholine doses. A dose which produced 70 "to 80 % of the maximum vasodepressant response effect was then selected and used for the remaining experiments.

After constant control results were obtained in the acetylcholine response, a dose injected the substance to be examined, whereupon

Θ09825 / 0874

A response to acetylcholine was found 30 s later. The response to acetylcholine was up then checked at 2 to 3 minute intervals. on In this way, both the effectiveness and the duration of action of the test substance to be examined could be determined will.

The effects of a number of different doses of each test compound were examined in each animal. Do everyone In the test, the response value to acetylcholine was allowed to return to the control level, before examining the effects of higher doses.

For use in the tests, each active ingredient was concentrated in distilled water of 10 mg / ml. All of the quaternary salts were freely soluble in water. Every connection was over administered in a dose range of 0.2 to 5> 0 mg / kg.

(2) Estimation of the antagonist strength

Gesamtileums strips of guinea pigs were placed in McEwen's solution saturated with carbogen (P _2/002 95: 5), gassed and was kept in a 10 ml organ bath at 37 ⁰ C. A tension of 1 g was applied to the tissue and the concentration-response curves _on acetylcholine were recorded cumulatively until a constant response was obtained.

The antagonist was then added to the bath in a certain concentration, after which, after a period of

609 8 25/0874

about 15 to 20 minutes for equilibration, further concentration-effect curves towards acetylcholine were added. This procedure was subsequently repeated using increasing concentrations of the antagonist.

The main curves were for the effects of acetylcholine recorded alone as well as for acetylcholine in the presence of various antagonist concentrations. The antagonism was determined from the dose ratios obtained in this way.

The acetylcholine concentration was determined by adding aliquots of stock solutions containing 0.1, 1, 10 and 100 / Ug / ml acetylcholine increased. The antagonist became dissolved in water to a stock solution with a concentration of 10 "" ^ M. This solution was subsequently Drawn in the bath to conduct the antagonist tests at concentrations of 10 "M and 10 M.

Results

I. d, lp-Cyclopentylphenylacetoxymethyltriethylammonium- chloride;

(1) guinea pig ileum - pAg = 8.0, atropine below same conditions pA2 = 8.6.

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(2) Acetylcholine Antagonist Effect on Cat Blood Pressure

Concentration
tion *
(mol-kg) effectiveness 1
O 3
18th 5
55 7th
82 9
100 18th
33 22nd
65 27
73 31
95 37
100 Time (min)
% Response ⁸ " 3.7 x 10 " ⁸ 1
O 3
O 6th
O 12th
18th 15th
36 Time (min)
% Responding ⁸ 3.7 x 10 " ⁷

a) Percentage of response to a dose of acetylcholine (0.05 / µg «kg ~) compared to the same dose in the absence of the antagonist.

II. D, 1- et -Cyclopentylphenylacetoxytaethyl-1 -methylmorpholiniumchlorid

(1) acetylcholine antagonist effects; on the blood pressure of cats

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Concentration
tion _Λ
(mol'kg ") effectiveness 1
0 VJI VN 4th
82 5
90 9
100 17th
59 21
73 25th
82 29
100 Time (min)
% Response ⁸ " 5.7 x 10 ~ ⁸ 1
O 4th
0 6th
0 10
23 13th
50 Time (min)
% Response ⁸ " 5.7 x 10 ~ ⁷

a) Percentage of response to a dose of acetylcholine
(0.05 µg «kg) compared to the same dose in the absence of the antagonist.

III. d, l-Ol -Cyclohe ^ qylphenylacetoxymethyltriethylammonium- chloride

(1) Acetylcholine Antagonist Effect on Cat Blood Pressure

Concentration
tion .
(mol «kg ~) 1
0 2
0 4th
50 effectiveness 6th
67 8th
83 10
100 co co I
ν O- j 21
93 24
100 Time (min)
% Response ⁸ " 5> 4 · 10 ~ ⁸ 1
0 3
0 6th
0 9
0 12th
43 15th
60 Time (min)
% Speak to 5.4. 10 " ⁷

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- yc-

a) Percentage response to an acetylcholine dose (0.05 / ug »kg ~) compared to the same dose in devi opposition of the antagonist.

IV. D, 1-ol-CyolopentylphenylacetoagTmethyl-i-methyl- pyrrolidinium chloride

(1) Guinea pig ileum same conditions

= 8.8, atropine below = 8.6.

(2) Acetylcholine Antaconist Effect on Cat Blood Pressure

Concentration
tion.
(mol.kg-) effectiveness 1
0 2
0 5
0 9
0 13th
31 18th
63 23
63 28
69 33
81 CO VN
CO CO 44
88 Time (min)
% Response ⁸ 5.4. 10 ' ⁹ 1
0 2
0 4th
67 7th
1OC Time (min)
% Response ⁰ 5.4. 10 " ⁸

a) Percentage of response to a dose of acetylcholine (0.02 / ug.kg ") compared to the same dose in the absence of the antagonist.

When using the other compounds according to the invention in the above-mentioned biological investigations

8Θ9825 / 0874

substantially the same results were obtained.

The dose and dosage form can vary both with regard to the individual doses and with regard to the daily doses vary depending on the requirements and the size of the organism being treated. Although the dose administered is not subject to any particular restrictions, it will usually correspond to an effective amount of the active ingredient, about its desired pharmacological and physiological effect, here mainly the antisecretory Effect, to achieve. To suppress gastric secretion, for example in the case of oral administration, a Dose range from 0.05 "to 10 mg / kg body weight per day sufficient. When administered topically to suppress perspiration, 0.01 to 5 is normally sufficient Wt .-% off.

For oral administration, for example in the form of tablets or capsules, the compounds according to the invention can be used in an anticholinergic, antisecretory Effectively effective amount with orally administrable, non-toxic, pharmaceutically acceptable inert carriers such as Lactose, starch (pharmaceutically pure), dicalcium phosphate, calcium sulfate, kaolin, mannitol and powdered sugar combined will.

The active ingredients or agents according to the invention can also if necessary also contain suitable binders, lubricants, disintegrants and / or coloring agents. Typical Binders include starch, gelatine, sugars such as cane sugar, molasses and lactose, natural and synthetic Gums such as acacia, sodium alginate, Irish moss extract, Carboxymethyl cellulose, methyl cellulose,

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Polyvinylpyrrolidone, Polyäthylenengiy _C ol, ethyl cellulose and waxes.

Typical lubricants for use in such dosage forms are, for example, boric acid, sodium benzene, sodium acetate, sodium chloride, leucine and polyethylene glycol, the substances mentioned being merely exemplary. Suitable disintegrants are, for example, starch, methyl cellulose, agar, bentonite, cellulose, alginic acid, guar gum, citrus pulp, carboxymethyl cellulose and sodium lauryl sulfate, the substances mentioned also being merely exemplary. If desired, conventional, pharmaceutically suitable dyes, for example the S ¹ DSiC standard dyes, can also be incorporated into the active ingredients or compositions according to the invention.

In the case of topical formulations for topical administration, the compounds according to the invention can likewise can also be combined with other suitable carrier materials, which can be used, for example, in the Armpit suitable. The carriers can be solid, liquid or as aerosols. For the purposes mentioned above suitable carriers can, for example, from the publication Remington's Pharmaceutical Sciences, 14th edition, 197O, as well as the publication by H. D. Goulden et al, Cosmetics, Science and Technology, Interscience Publishers 1957, PP. 5, 717-731, 826-829, 1016, 1211, 1255 or 1266, can be easily removed.

The invention is not limited to the compounds given by way of example and the information given in the examples limited, since the inventive concept also includes equivalent developments.

909825/0874

Claims (1)

BEETZ-LAMPRECHT-BEETZ Steinsdorfstrasse 10 D-8000 Munich 22 Telephone (089) 2272 01 - 22 7244 - 29 5910 Telex 522048 - Telegram Allpaterit Munich ol45-29.o63P PATENT LAWYERS Dipl.-Ing. R. BEETZ sen. Dipl-Ing. K. LAMPRECHT Dr.-Ing.R BEETZ jr Lawyer Dipl.-Phys. Dr. jur. U. HEIDRICH Dr.-Ing.W TIMPE Dipl Ing.J.SIEGFRIED Priv.-Doz. Dipl.-Chem. Dr. ret. nat. W. SCHMITTFUMIAN Dec 15, 1978 Claims Connections of the formulas C - C - X - CH - I Il R /, and IU - (D C - C. - X -CH- I. Il \ O in which mean: Ή ~ ^ a tertiary amine, IT ^ ¹ an unsaturated area, ^B0D ) Si 78 AT 207 BOD / ¹ i7nu $ 09825/0874 Original inspected R, and R _2t simultaneously or independently Η, an open-chain C ₁ - to Cn- Alkyl group,
a cycloalkyl or cycloalkenyl group with up to 8 carbon atoms, a C ₁ - to Cg -alkoxyalkyl group, a C ₁ - to Cn-acyloxyalkyl group, a C ₁ - to Cg-haloalky group, a C ₁ - to Cn-carboxyalkyl group, a C ₂ - to Cn-alkenylphenyl group, an aryl group or an _{aryl group substituted with halogen, C 1} - to C ^ -O-alkyl, O-acyl, nitro, carboxyl or carbethoxy, -CH ₂ -OH, -CH ₂ -OCOR ₁ ¹ , where R ₁ 'is the same as below R ₁ or -CH ₂ -ONO, -OH, Halogen. , -OCOR ₁ and two with R ₁ as below R ₂ , R, and Rj. or -ONO ₂ , are whereby at least the substituent ducks Rp, R, Rj. Of hydrogen different 5 and together have at least 5 carbon atoms or R ₂ , R ^ and Rjj together with the ot-c atom to which they are bonded form a condensed polycarbocyclic or polyheterocyclic ring, R _{1 the} same as Rp, R, or Rj., X -0- or -S- and Y is halogen or an equivalent organic or inorganic monovalent anion. 909825/0874 2. Compounds of formulas (I) and (II) according to claim 1, characterized in that X is -O-. 3. Compounds of E formulas (I) and (II) according to claim 1 or 2, characterized in that Ro ₁ R _z and R ^. Are aryl groups, 4 ·. Connections according to claim 3 »characterized in that that the aryl groups are phenyl groups. 5. Compounds according to claim 1 or 2, characterized in that that at least one of the substituents Rp, R, and R ^ is a cycloalkyl group. 6. Compounds according to claim 1 or 2, characterized in that at least one of the substituents Rp, RZ and R _{1 is} a cycloalkenyl group. 7- Compounds according to claim Λ or 2, characterized in that R ₂ , Rj and R ^ together with the tf-C atom to which they are bonded form a condensed polycarbocyclic ring. 8. Compounds according to claim 7 »characterized in that that the polycarbocyclic ring is an adamantyl group. 9. Compounds according to claim 1 or 2, characterized in that at least one of the substituents Rp, R, and R _{2 is} hydrogen. 10. Compounds according to any one of claims 1 to 9 »thereby characterized in that the amine portion is a pyrrolidine ring 80982570874 having. 11. Compounds according to any one of claims 1 to 9, characterized in that the amine part is a quinuclidine ring having. 12. Compounds according to any one of claims 1 to 9i characterized in that the amine portion has an azirine ring. 13. Compounds according to any one of claims 1 to 9, characterized characterized in that the amine portion has a pyrrole ring. 14. Compounds according to any one of claims 1 to 9, characterized characterized in that the amine portion has an imidazole ring. 15. Compounds according to any one of claims 1 to 9, characterized characterized in that the amine part has a pyrazzo ring. 16. Compounds according to any one of claims 1 to 9i characterized in that the amine portion has a pyridine ring. 17. Compounds according to any one of claims 1 to 9 »thereby characterized in that the amine portion has a pyrazine ring. 18. Compounds according to any one of claims 1 to 9 ₅ , characterized in that the amine part is a pyridazine ring §09825 / 0874 having. 19. Compounds according to one of claims 1 to 9, characterized characterized in that the amine portion has a pyrimidine ring. 20. Compounds according to any one of claims 1 to 9, characterized characterized in that the amine portion has an isoindole ring. 21. Compounds according to any one of claims 1 to 9, characterized in that the amine part has an indole ring. 22. Compounds according to any one of claims 1 to 9 »thereby characterized in that the amine portion has a quinoline ring. 23. Connections according to one of claims 1 to 9? through this characterized in that the amine part is an isoquinoline ring having. 24. Compounds according to any one of claims 1 to 9i characterized in that the amine moiety is a phthalazine ring having. 25. Compounds according to any one of claims 1 to 9 _5, characterized in that the amine part has a quinox ^ linring. 26. Compounds according to any one of claims 1 to 9, characterized in that the amine part is a quinazoline ring 90982 5/0874 having. 27. Compounds according to one of claims Ί to 9> characterized in that the AminbM.l is a phenazine ring having. 28. Compounds according to any one of claims 1 to 9 »thereby characterized in that the amine portion has an isothiazole ring. 29. Compounds according to any one of claims 1 to 9 »thereby characterized in that the amine moiety is a phenothiazine ring having. 30. Compounds according to any one of claims 1 to 9, dsdurch characterized in that the amine portion is an isoxazole ring; 31. Compounds according to any one of claims ^Λ > to 9, characterized in that the amine part has a furazan ring. 32 «, compounds according to one of claims 1 to 9, characterized characterized in that the amine moiety is a morpholine ring aufv / ej st. 33. Compounds according to any one of claims 1 to 9, characterized characterized in that the amjnteil is a tertiary aliphatic Amine is. 34 ·. Compounds according to any one of claims 1 to 335 characterized in that JL, is an alkyl group. 609825/0874 35 · Connections according to one of claims 1 to 33 »thereby characterized in that R ^ eats hydrogen. 36. Compounds according to any one of claims 1 to 33 »characterized in that Rx] is an alkoxyalkyl group is. 37 · Connections according to one of claims 1 to 33 »thereby characterized in that R ^ is an acyloxyalkyl group is. 38. Compounds according to any one of claims 1 to 33 »thereby characterized in that R ^ is a carboxyalkyl group is. · Ί - [d, 1- el -Cyclopentylphenylacetoxymethyl] -1 -methyl- pyrrolidinium chloride as a compound according to claim 40. 1- [d, l-oL-Cyclopentylphenylacetoxymethyl] -1.2-di- methylpyrrolidinium chloride as a compound according to claim 1, 41. 1- [d, 1- oL-Cyclopentylphenylacetoxymethyl] -3-ethoxy- carbonylpyridipium chloride as a compound according to claim 1. 42. 1- [d, l- d-Cyclopentylphenylacetoxymethyl] -tri ^ propoxy- ethylammonium chloride as a compound according to claim 43. 1- [d, l- oL-Cyclohexylphenylacetoxymethyl] -1-methyl- pyrrolidinium chloride as a compound according to claim S09825 / 0S74 44-, i- ^ jl-a-Cyclohexylplienylacetoxymethyl] -1.2-di- methylpyrrolidinium chloride as a compound according to claim 1. 4-5. 1- [d, l-2-phenylbutyryloxytnethyl] -J-methyliraidazolium- chloride as a compound according to claim 1. 46. 1- [d, 1-2-phenylbutyryloxymethyl] -3-acetoxychin- clidinium chloride as a compound according to claim 1. 4-7. 1- 1 d, 1-2-phenylbutyryloxymethyl] -tri ^ propoxyethyl- ammonium chloride as a compound according to claim 1. 48. 1- [d, 1-2-methylbutyryloxymethyl] -1-methylmorpholinium- chloride as a compound according to claim 1. 4-9. Ί - [d-ct -Gyclohex-E-enylphenylacetoxymethyl] -1 -methyl- -pyrrolidinium chloride as a compound according to claim 1.- 50. 1- [d-oL-Cyclohex-2-enylphenylacet02qjTethyl] -3-ethoxy- carbonylpyridinium chloride as a compound according to claim l. 51. 1- [l- oL-Cyclopropylphenylacetoxymethyl] -1-methyl- -pyrrolidiniumcbJLorid as a compound according to claim l. 52. 1- [l-OL-Cyclopropylphenylacetoxymethyl] -1.2-dimethyl- pyrrolidinium chloride as a compound according to claim * ■ · Ί - [l- cL-Cyclopropylphenylacetoxymethyl] -tri-propoxy- -äthylammoniumchlorid as a compound according to claim 1, 609825/087 * - Q - 54. Process for the preparation of the compounds I and II according to one of claims 1 to 53, marked by (a) Implementation of a compound of the general formula ? 2 S Pl R, - C - C - X - CH - Hai with R ₁ , R ₂ , R ₁ , R 1 J and X as above and Hal = halogen with a tertiary amine (N ^) or an unsaturated one Amine (N ^) or (b) Implementation of a tertiary amine (N ^) or one unsaturated amine (N ~ Ξ ^) with a compound the general formula R ₂ 0 R ₇ -CC- shark
3 ι ^R 4
with Rp, R ^, Rk and Hai as above and subsequent reaction of the resulting reaction mixture with an aldehyde of the formula HC = O with R ₁ as above
or (c) Quaternization of a compound of the general formula 809825/0874 R ₀ 0 R ₀ R ₃ -CCX-CH-NC,
K in the R., R _? , R ,, Rj, and X the same as
above and N <[the remainder of a secondary
Amines mean whereupon the resulting compound of the formula I or II, in which Y is halogen, is exchanged if necessary of the anion is subjected when a compound those of the formulas I and II is sought, in Y is no halogen. 909825/0874 55. The method according to claim 5 * 1 for the production of compounds of formula I, characterized in that one of the process variants (a), (b) and (c) is applied. 56. The method according to claim 5 ^ for the production of compounds of formula II, characterized in that one of the process variants (a), (b) and (c) is used will. 57. The method according to claim 5 ¹ I for the preparation of compounds of the formulas I or II, in which X = O, characterized in that one of the process variants (a), (b) and (c) is used, where X = O is. according to claim 5 ^ 58. Process / for the preparation of compounds of the formulas I. or II, in which at least one of the substituents Rp, R, and R _{1 is} aryl, characterized in that one of the process variants (a), (b) and (c) is used, where at least one of the substituents R ₂ , R? and Rj, is aryl. 59.Verfahren according to claim 58, characterized in that the aryl group is phenyl. 60. The method according to claim 5 ^ for the preparation of compounds of the formulas I or II, in which at least one of the substituents R ₂ , R-, and Rj, is cycloalkyl, characterized in that one of the process variants (a), (b) and (c) is applied, where at least one of the substituents R _? , R-, and Rj, is cycloalkyl. 61. The method according to claim 54 for the preparation of compounds of the formulas I or II, in which at least one of the substituents R ₂ , R, and Rj. Is cycloalkenyl, characterized in that one of the process variants ÖÖ9825 / 087 * - ioa - (a), (b) and (c) is used, where at least one of the substituents Rp, R, and R ₁ , is cycloalkenyl. 62. The method according to claim 5 ^ for the preparation of compounds of the formulas I or II, in which Rp, R, and R ₁ . together with the Λ-C atom to which they are bonded form a condensed polycarbocyclic ring, characterized in that one of process variants (a), (b) and (c) is used, the substituents Rp, R, and Rj. Together with the ot-c atom to which they are attached form a condensed polycarbocyclic ring. 63. The method according to claim 62, characterized in that the condensed polycarbocyclic ring is adamantyl. 6h. Process according to Claim 5 ^ for the preparation of compounds of the formulas I or II in which at least one of the substituents Rp, R- and R _{1 is} hydrogen, characterized in that one of the process variants (a), (b) and ( c) is used, where at least one of the substituents Rp, R, and R ^ is hydrogen. 65. The method according to claim 5 ^ for the preparation of compounds of the formula I in which the amine part has a pyrrolidine ring,
marked by (a) Implementation of a compound of the general formula R ₀ 0 R ₁
i 2 π ι 1 R ₃ -CCX-CH- Hai with R ₁ , R ₂ , R ,, R ₂ ,, X and Hai as in claim 5 ^ - 10b §09825 / 0874 with a pyrrolidine
or (b) Reaction of a pyrrolidine with a compound of the general formula R ₀ O ι ² Il R ₃ -CC- shark with R ", R", Rj. and Hai as in claim 5 and subsequent reaction of the resulting reaction mixture with an aldehyde of the formula Fi HC = O with R. as in claim 54 or (c) quaternizing a compound of the formula R ₉ 0 R ₁ I 2 κ ι 1 ^ RCCX-CH-NJ ^R with R ^, Rp, R ,, Rj, and X as in claim and R ₁ - = H or C ₁ - to Cg-alkyl by treatment with an alkyl halide, if a 1-alkylpyrrolidine is desired, whereupon the resulting compound in which Y represents a halogen, if necessary, if a compound is desired in which Y is not halogen, is subjected to an exchange of the counterion. - 10c - §09825 / 0874 - .108 - 66. The method according to claim 5 ^ for the production of compounds of formula I, in which the amine part has a quinuclidine ring, marked by (a) Implementation of a compound of the general formula R ₀ OR ₁ R ₃ -CCX-CH- Hal with R ₁ , R ₀ , R_, Rj., X and Hai as in claim 5 * 1 with a quinuclidine
or (b) Reaction of a quinuclidine with a compound of the general formula R ₀ O
i 2 11 R, - C - C - shark
3 1 with Rp, R _7. , Rj. and Hal as in claim 5 ^ and then reacting the resulting reaction mixture with an aldehyde of the formula HC = O
with R. as in claim 5 ^ » whereupon the resulting compound, in the formula of which Y is halogen, if necessary, if a compound is sought, in whose formula Y is not halogen, is subjected to an exchange of the counterion. - 1Od - 8Θ9825 / 0874 67. The method according to claim 5 ^ for the preparation of compounds of the formulas I or II, in which the Arainteil an azirine ring, pyrrole ring, imidazole ring, pyrazole ring, pyridine ring, pyrazine ring, pyridazine ring, pyrimidine ring, isoindole ring, indole ring, quinoline ring, isoquinoline ring, phthalazine ring, quinoxaline ring , Quinazoline ring, phenazine ring, isothiazole ring, phenothiazine ring, isoxazole ring, furazan ring or morpholine ring, marked by (a) Implementation of a compound of the general formula ι 2 H jl R, -C-C-X-CH- Hai 3 ι with R., R ", R", R _1. , X and Hai as in claim with one of azirines, pyrroles, imidazoles, pyrazoles, pyridines, pyrazines, pyridazines, Pyrimidines, isoindoles, indoles, quinolines, isoquinolines, phthalazines, quinoxalines, quinazolines, Phenazines, isothiazoles, phenothiazines, isoxazoles, furazans and morpholines Amine or (b) Implementation of one of azirines, pyrroles, imidazoles, pyrazoles, pyridines, pyrazines, pyridazines, Pyrimidines, isoindoles, indoles, quinolines, isoquinolines, Phthalazines, quinoxalines, quinazolines ^ phenazines, isothiazoles, phenothiazines, isoxazoles, Furazans and morpholines selected amine with a compound of the general formula h 9 ■ -C- shark ¹¹ - 1Oe - 909825/0874 with R ₂ , R, and R ₁ ^ as in claim 54 and then reacting the resulting reaction mixture with an aldehyde of the formula HC = O with R. as in claim 54 or (c) quaternization of the corresponding compound of the formula R ₀ O R.
I 2 i | ι 1 R ₃ -CCX-CH-Z, R ₄ in which mean: R ₁ , R _? , R ^, R ₁ , and X the same as in claim 54 and Z the radical of an azirine, pyrrole, imidazole, pyrazole, isoindole, phenothiazine or morpholine by treatment with an alkyl halide, if a corresponding 1-alkylazirine, 1-alkylpyrrole, 1-alkylimidazole, 1-alkylpyrazole, 2-alkylisoindole, 10-alkylphenothiazine or N-alkylmorpholine is sought, whereupon the resulting compound, in the formula of which Y is a halogen, is subjected to an exchange of the counterion when a compound ₃ in the formula of which Y is not halogen is desired. 68. The method according to claim 54 for the production of connec- a fertilizer of the formula I, whose amine part / tertiary aliphatic - 1Of 809825/0874 has cal amine, characterized 'by (a) Implementation of a compound of the general formula R ₉ OR ₁ R, - C - C - X - CH - Hai j j with R., R ", R", Ru, X and Hai as in claim \ with a tertiary aliphatic amine or (b) Reaction of a tertiary aliphatic amine with a compound of the general formula R-ι ² Il Ri-CC- Hai j i with Rp, R ,, R ^ and Hai as above and then reacting the resulting reaction mixture with an aldehyde of the formula h HC = O with R. as in claim or (c) Quaternizing a compound of the general formula R ₂ 0 R ₁ R ₃ -CCX-CH- N ^ with R ₁ , Rp, R ,, R ₁ , and X as above and Nd. = radical of a secondary aliphatic amine, 909825/0874 - log - whereupon the resulting compound, in the formula of which Y is halogen, is exchanged if necessary of the counterion is subjected when a compound is desired, in the formula Y does not contain halogen represents. 69. The method according to claim 54 for the preparation of compounds of the formulas I or II, in which R _{1 represents} alkyl, hydrogen, alkoxyalkyl, acyloxyalkyl or carboxyalkyl, characterized in that one of the process variants (a), (b) and (c) is used, where FL is alkyl, hydrogen, alkoxyalkyl, acyloxyalkyl or carboxyalkyl. 70. The method according to claim 54 for the preparation of l- [d, l-X-cyclopentylphenylacetoxymethyl] -1-methylpyrrolidinium chloride, characterized in that chloromethyl-d, l-oC-cyclopentylphenyl acetate reacted with 1-methylpyrrolidine will. 71. The method according to claim 54 for the preparation of l- [d, l-a-Cyclopentylphenylacetoxymethylj-l ^ -dimethylpyrrolidiniumchlorid, characterized in that chloromethyl-d, l-cyclopentylphenyl acetate is reacted with 1,2-dimethylpyrrolidine. 72. The method according to claim 5 ^ for the preparation of l-Qd, l-a.-Cyclopentylphenylacetoxymethyl] -3-ethoxycarbonylpyridinium chloride, characterized in that chloromethyl-d, l- «x- reacted cyclopentylphenyl acetate with 3-ethoxycarbonylpyridine will. 73. The method according to claim 5 ^ for the preparation of l- [d, l-0i.-Cyclopentylphenylacetoxymethyl] - tripropoxyethylammonium 009825/0874 Chloride, characterized in that chloromethyl-d, l - «> cyclopentylphenyl acetate reacted with tripropoxyethylamine will. 7 ¹ year process for the preparation of 1- [d, l - & - cyclohexylphenylacetoxymethyl] -l-methylpyrrolidinium chloride, characterized in that chloromethyl-djl-oc-cyclohexylphenyl acetate is reacted with 1-methylpyrrolidine. 75 · Process according to claim 54 for the preparation of l- [d, l-0t-cyclohexylphenylacetoxymethyll-1,2-dimethylpyrroldinium chloride, characterized in that chloromethyl-d, l- <xcyclohexylphenyl acetate reacted with 1,2-dimethylpyrrolidine will. 76. The method according to claim 54 for the preparation of l- [d, l-2-phenylbutyryloxymethyl] -J-methylimidazolinium chloride, thereby characterized in that chloromethyl-d, l-2-phenylbutyrate is reacted with 3-methylimidazole. 77 · Process according to claim 54 for the preparation of l- [d, l-2-phenylbutyryloxymethyl] ^ - acetoxyquinuclidinium chloride, characterized in that chloromethyl-d, l-2-phenylbutyrate is reacted with 3-acetoxyquinuclidine. according to claim 54 78. Process / for the preparation of l- [d, l-2-phenylbutyryloxymethyl- ' tripropoxyethylammonium chloride, characterized in that chloromethyl-d, l-2-phenylbutyrate with tripropoxyethylamine is implemented. 79 · The method according to claim 54 for the preparation of l- [d, l-2-methylbutyryloxymethyl] -l-methylmorpholinium chloride, characterized in that chloromethyl-d, l-2-methylbutyrate is reacted with 1-methylmorpholine. - 10i 609825/0874 according to claim 54 80. Process / for the preparation of l- [d-oc-Cyclohex-2-enylphenylacetoxymethyll-l-methylpyrrolidinium chloride, characterized in that chloromethyl-d-oc-cyclohex-2-enylphenyl acetate is reacted with 1-methylpyrrolidine. 81. The method according to claim 54 for the preparation of 1-Qd-iX-cyclohex-2-enylphenylacetoxymethyl] -3-ethoxycarbonylpyridinium chloride, characterized in that chloromethyl-d-oC-cyclohex-2-enylphenyl acetate is reacted with 3-Ä'thoxycarbonylpyridin. 82. The method according to claim 54 for the preparation of i - [(l-o.-Cyclopropylphenylacetoxymethyll-l-methylpyrrolidinium chloride, characterized in that chloromethyl-l-ot ^ cyclopropylphenyl acetate is reacted with 1-methylpyrrolidine. 83. The method according to claim 54 for the preparation of 1 - [* (1-0O-CyclopropylphenylacetoxymethylJ-l ^ -dimethylpyrrolidinium chloride, characterized in that chloromethyl-1-ct-cyclopropylphenyl acetate is reacted with 1,2-dimethylpyrrolidine. 84. The method according to claim 54 for the production of 1-C Cyclopropylphenylacetoxymethyl] tripropoxyethylammonium chloride, characterized in that chloromethyl-1 - «.- cyclopropylphenyl acetate is reacted with tripropoxyethylamine. 85. Pharmaceutical agents, characterized by an effective amount of at least one compound according to one of Claims 1 to 53 86. Pharmaceutical agents according to claim 85, characterized by a content of! - [djl-öc-Cyclopentylphenylacetoxymethyi] -1-methylpyrrolidinium chloride. 809825/0874. _1O j - - JAT-21 87. Pharmaceutical agents according to claim 85> characterized by a content of 1-Ldjl-ot-cyclopentylphenylacetoxymethyl] -1,2-dimethylpyrrolidinium chloride. - 11 - 909825/0874 according to claim _8ü. Pharmaceutical ITittelV "characterized by a content to 1- £ d, l- -l-Cyclopentylphenylacetoxymethylj-3- -ethoxycsrbonylpyridinium chloride. according to claim. 85 . Pharmaceutical agentsX characterized by a content to 1- [~ d, l-oL-Cyclopentylphenylacetoxymethyl] -tri- -propoxyethylammonium chloride. ^ nach_A η sρ ru ch_ Jfiy 90. Pharmaceutical agents ¹ , characterized by a content of i- ^ jl-oL-GyclohexylphenylacetoxymethylJ-i-
-methylpyrrolidinium chloride. , nach_ claim .. JBjL ^ 91. Pharmaceutical agents characterized by a content an 'i-fdjl-'jL-CyclohexylphenylacetosqyTnethyl] -1.2- -dimethylpyrrolidinium chloride. according to ans pruch 85 / 92. Pharmaceutical agents ^, characterized by a content of 1- [d, l-2-phenylbutyryloxymethyl] -3-methyl-
-imidazolium chloride. _v n oh Anspruc h ^ 85 M5. Pharmaceutical MltteT, characterized by a content of Ί - [d, 1-2-phenylbutyryloxymethyl] -3-acetoxy-
-quinuclidinium chloride. see spuch_j5 ^
gh. Pharmaceutical agents ", characterized by a Ge content of 1- [d, 1-2-phenylbutyryloxymethyl] -tri-propoxy- ethylammonium chloride. ^ Claim 83.
Pharmaceutical center, indicated by a. Content of 1- [d, l-2-riethylbutyryloDq7methylJ-1-methyl- Θ09825 / 0874 -morpholinite chloride. _v according to claim 8 j5 ^ 96. Pharmaceutical agents · ^ characterized by a content to 1- [d-OL-Cyclohex-2-enylphenylaceto3qymethyl] -1- -methylpyrrolidinium chloride. jiach claim 85 ^ 97. Pharmaceutical Agents '', characterized by a content to 1- [d-oL-cyclohex-2-enylphenylacetoxymethyl] -3- ethoxycarbonylpyridinium chloride. jnach_A nspruch 85_ ^ 98. Pharmaceutical means ^ characterized by a content an i-J ^ l-oL-Cyclöpropylphenylacetoxymethyl] -1- -methylpyrrolidinium chloride. according to claim 8 ^ , 99. Pharmaceutical means ^ "characterized by a content an i-fl-oL-Gyclopropylphenylacetoxymethyl] -1.2- -dimethylpyrrolidinium chloride. according to claim 85, 1OQ, Pharmaceutical Agents, characterized by a content to i-fl-GL-Cyclopropylphenyiacetoxymethyl] -tri- -propoxyethylammonium chloride. 101. Antiperspirants for external use in the Personal hygiene, characterized in that they contain an effective amount of at least one compound according to one of Claims Λ to 53, together with customary auxiliaries and / or carriers. 102. "Procedure for the local prevention of perspiration in warm-blooded animals and humans, characterized in that an effective amount of at least one 809825/0874 A compound according to any one of claims 1 to 53 topically is applied. 105. The method according to claim Iu ^, characterized in that that an antiperspirant according to claim 73 is used. · 10 * 1. The method of claim 102 or 103, characterized in that the active ingredient in an amount of 0.01 to 5 wt -% is applied.. 809825/0874