US2479843A - 1-alkylpiperidyl-4-benzhydryl ethers, acid salts thereof and their preparation - Google Patents

1-alkylpiperidyl-4-benzhydryl ethers, acid salts thereof and their preparation Download PDF

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US2479843A
US2479843A US30735A US3073548A US2479843A US 2479843 A US2479843 A US 2479843A US 30735 A US30735 A US 30735A US 3073548 A US3073548 A US 3073548A US 2479843 A US2479843 A US 2479843A
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benzhydryl
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Knox Lawrence Howland
Kapp Roland
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Nopco Chemical Co
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    • CCHEMISTRY; METALLURGY
    • C07ORGANIC CHEMISTRY
    • C07DHETEROCYCLIC COMPOUNDS
    • C07D211/00Heterocyclic compounds containing hydrogenated pyridine rings, not condensed with other rings
    • C07D211/04Heterocyclic compounds containing hydrogenated pyridine rings, not condensed with other rings with only hydrogen or carbon atoms directly attached to the ring nitrogen atom
    • C07D211/06Heterocyclic compounds containing hydrogenated pyridine rings, not condensed with other rings with only hydrogen or carbon atoms directly attached to the ring nitrogen atom having no double bonds between ring members or between ring members and non-ring members
    • C07D211/36Heterocyclic compounds containing hydrogenated pyridine rings, not condensed with other rings with only hydrogen or carbon atoms directly attached to the ring nitrogen atom having no double bonds between ring members or between ring members and non-ring members with hetero atoms or with carbon atoms having three bonds to hetero atoms with at the most one bond to halogen, e.g. ester or nitrile radicals, directly attached to ring carbon atoms
    • C07D211/40Oxygen atoms
    • C07D211/44Oxygen atoms attached in position 4
    • C07D211/46Oxygen atoms attached in position 4 having a hydrogen atom as the second substituent in position 4

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  • This invention relates to antihlstaminic agents and to a new class of compounds having highly effective antlhistaminic properties.
  • each of these eight com.- pounds contains one or the other of two rather similar groups.
  • six of the eight compounds contain the group NiiN I l and that the other two compounds contain the group Feinberg stated in his article that as far as was known at that time, the antihistaminic agents operate by competing with liberated histamine in attaching to receptor cells. Since all of the effective antihistaminic agents to date contain one or the other of two similar chemical groups, it is reasonable to assume that one or the other of these groups must be present for any compound to be an eiiicient antihistaminic agent, and that the antlhistaminic agents heretofore known attach to the receptor cells through or by means of one of these two groups.
  • R is an alkyl group containing from 1 to 4 carbon atoms, i. e. methyl, ethyl, propyl, and butyl and propyl and butyl isomers, and hydrohalide salts of such compounds are highly effective antihistazminic agents.
  • the preferred antihistaminic compounds of our invention are 1-methyl-piperidyl-4-benzhydry1 ether and the hydrohalide salts thereof.
  • the compounds of our invention may be prepared by reacting a l-alkyli-piperidinol wherein the alkyl group contains from i to 4 carbon
  • These new compounds may also be prepared by reacting l-alkyl-i-haloplperidines with benzhydrol or the sodium or potassium derivatives thereof or by reacting sodium or potassium derivatives of 1-alkyl-4-piperldinols with benzhydryl halides.
  • the reaction may be carried out by heating the desired reactants together until the desired ether compound is formed.
  • the reaction is carried out in the presence of some inert solvent such as an aromatic or aliphatic hydrocarbon solvent or a high boiling aliphatic ether.
  • inert solvent such as an aromatic or aliphatic hydrocarbon solvent or a high boiling aliphatic ether.
  • compounds such as benzene, toluene, xylene, heptane, octane, nonane, decane, dipropyl ether, dibutyl ether, diamyl ether, etc., may all be employed.
  • the particular inert solvent which is used is not critical since its only function is to allow for a more emcient interaction of the reactants.
  • any organic solvent such as those just mentioned which has a boiling point of about C. or above and which will not enter into reaction with either of the reactants being employed in preparing the desired compounds or with the desired compounds themselves may be used as a solvent in which to carry out the reaction.
  • the amount of inert solvent, if any, which is employed is suitably equal to or slightly in excess of the amount of reactants being used.
  • an excess of the l-alkyl-i-plperidinol compound may be employed to serve as a solvent medium for the reaction or, if desired, similar heterocyclic compounds such as pyridine, etc, may be utilized as a solvent medium tor the reaction.
  • the reaction mixture may be heated under pressures greater than atmospheric if desired. Usually. it is preferred to heat the reaction mixture at the reflux temperature of the lowest boiling component thereof.
  • the two compounds which are to be reacted in each case to prepare one of the new compounds of our invention may be reacted in a mol to mol ratio or, if desired, an excess of the basic heterocyclic compound may be employed. If a mol to mol ratio of the reactants is used, the ether will be produced, at least to some extent, in the form of its hydrohalide salt. Preferably at least a molar excess of the basic heterocyclic compound is employed in carrying out the preparation of the compounds of our invention.
  • One of the reasons for this is that .by having such an excess of a basic compound present any free hydrogen halide produced by the reaction will be neutralized by such excess basic compound and reaction mixture to neutralize any hydrogen halide which is formed.
  • the reaction should preferably be carried out under substantially anhydrous conditions in order to obtain the most favorable yields and therefore it is preferable to employ only substantially anhydrous reactants and solvents.
  • reaction mass will separate into two layers if an excess of a piperidinol or similar basic compound has been employed, the upper phase containing the desired benzhydryl ether compound. If an inert solvent such as xylene, toluene or one of the other;
  • the lower phase of the reaction mixture will be made up of the excess piperidinol or similar basic compound, if any. If no inert solvent was utilized in the carrying out of the reaction, a volume of such a solvent equal to about the volume of the reaction mixture may be added thereto so as to aid in separating the desired benzhydryl ether compound from the rest of the reaction mixture.
  • any inert solvent in that phase is removed therefrom, e. g., by distillation under reduced pressure.
  • the crude benzhydryl ether may then be purified by dissolving it in an excess of an aqueous acid solution of medium strength, e. g. 20% hydrochloric acid, and the aqueous acid solution then washed with some solvent such as ethyl ether to remove any non-basic impurities therefrom. If the reaction mixture does not separate into two phases, any inert solvent therein may be removed as by distillation under reduced pressure and the remainder of the reaction mix ture then admixed with an aqueous acid solution and the resulting mixture washed with a solvent such as ethyl ether to remove any nonbasic impurities.
  • medium strength e. g. 20% hydrochloric acid
  • the aqueous acid solution of the desired benzhydryl ether compound may be decolorized with activated carbon and the acid solution neutralized with a base such as aqueous ammonia.
  • the free benzhydryl ether compound will separate from the aqueous solution as an oily material and may be readily recovered by extraction with a solvent such as ethyl ether or a similar solvent.
  • the oily product may then be converted to a crystalline hydrohalide salt by dissolving the oily product in a solvent such as isopropanol and adding thereto an alcoholic, e. g., methanolic, ethanolic, etc., halide.
  • Ethyl ether may then be added to the acidified solution until a faint turbidity is observed.
  • the crystalline hydrohalide salt of the benzhydryl ether will soon separate and after recovery from the solution may be further purified by recrystallization from a small amount of a solvent such as i-propanol if
  • the reaction mixture separated into two phases with the upper phase containing the desired ether compound dissolved in xylene.
  • the lower phase consisted of the hydrobromide salt of the excess i-methyli-piperidinol.
  • the upper phase was separated from the lower phase and the desired benzhydryl ether recovered in the crude state by distilling of! the xylene under reduced pressure.
  • the crude benzhydryl ether was a clear reddish oil. It was dissolved in '75 m1.
  • the benzhydryl ether separated as an oily material and was removed from the aqueous mixture by extraction with three 50 ml. portions of ethyl ether. On evaporation of the ethyl ether from the ethyl ether solution, the benzhydryl ether was recovered as a pale yellow oil. The benzhydryl ether was dissolved in 60 ml.
  • the compounds of our invention manifest antiasthmatic action when tested on animals.
  • the compound having the formula 8 The compound having the formula 4.
  • the compound having the formula carbons and aliphatic ethers having boiling points of at least 80 C.. and the reaction mixture is heated at the reflux temperature of the inert solvent.
  • reaction is carried out in the presence of an inert solvent selected from the class consisting of aliphatic and aromatic hydrocarbons and aliphatic ethers having boiling points of at least 80 C., and the reaction mixture is heated at the reflux temperature of the inert solvent.
  • an inert solvent selected from the class consisting of aliphatic and aromatic hydrocarbons and aliphatic ethers having boiling points of at least 80 C.

Description

Patented Aug. 23, r949 1 ALKYLPIPERIDYL 4 BENZHYDRYL ALTS THEREOF AND THEIR PREPARATION Lawrence Howland Knox, Katonah, N. Y., and Roland Kapp, Newark, N. 1., assignors to Nopco Chemical Company, Harrison, N. J a corpora- ETHERS, ACID S tion of New Jersey No Drawing. Application June 2, 1948, Serial No. 30,735
8 Claims. (Cl. 260-293) This invention relates to antihlstaminic agents and to a new class of compounds having highly effective antlhistaminic properties.
It is only in comparatively recent years that medical science has succeeded in developing drugs which could be used satisfactorily in counteracting the painful, irritating and sometimes fatal effects of various types of allergic and similar disturbances such as food allergy, serum sickness, hayfever, asthma, migraine, urticaria, etc.
As a result of work carried out by numerous researchers, it has been rather definitely shown that occurrence of the above and similar disturbances may in practically all cases be traced, at least in part, to the liberation of histamine from a fixed state in certain of the body cells and the subsequent reaction of the liberated histamine upon other body cells as the histamine diffuses into surrounding tissues. It is believed that the histamine is released from its fixed state in the cells in which it is contained by the action upon such cells of various compounds which in many cases appear to be of a protein nature and which are usually referred to as allergens. These allergens are found in substances such as the pollen of various weeds, in foods such as strawberries, eggs, etc., in serums used in treating various diseases, etc.
At first it was believed that by injecting histamine into persons who were subject to allergies and similar disturbances a tolerance to histamine could be developed; however, it was found that such was not the case. Thereafter various researchers directed their efforts along the lines of developing drugs which would either destroy histamine or in some manner or other alleviate its ill effects. In recent years several drugs have been developed which have been found to be rather effective antihistaminic agents. All of the effective antihistaminic compounds so far developed seem to counteract the effect of histamine by, in some manner or other, attaching themselves to the various body cells which would be affected by the liberated histamine and either preventing such histamine from itself attaching to such receptor cells or displacing the histamine if it is already attached to such cells.
In the Journal of The American Medical Association, 132, 702 (1946), there is an excellent article by Feinberg in which he discusses the antihistaminic agents known at that time and the various results which have been obtained from the use thereof. According to his article the tour compounds which have been found to be the most elective are:
N phenyl-N' benzyl-N-dimethylethylenedlamine H @i H H ,H s \aam Q/ A A \CH| N-p-methoxybenzyl-N-dimethylaminoothyl a aminopyrldino Q 1i i on Beta-dimethylaminoethyl benzhydryl ether hydrochloride and N a pyrldyl-N' benzyl-Ndlmethylethylenediamine i t N 2-isopropyl-5-methylphencxyethyldlethylamine C H! C H;
I l- M Olin t if N-phenyl-N-ethyl-N' dlethylothylencdiamine N phenyl-N' ethyl-N-dimethylethylenediamine CaHt Another compound which has recently been found to have antihistaminic properties is the hydrochloride salt of N,N-dimethyl-N' 2-theny1)-N- (2-pyridyl) -ethylenediamine i L i i in... Q i i a.
From the comparison of the above formulae it will be seen that each of these eight com.- pounds contains one or the other of two rather similar groups. Thus it will be seen that six of the eight compounds contain the group NiiN I l and that the other two compounds contain the group Feinberg stated in his article that as far as was known at that time, the antihistaminic agents operate by competing with liberated histamine in attaching to receptor cells. Since all of the effective antihistaminic agents to date contain one or the other of two similar chemical groups, it is reasonable to assume that one or the other of these groups must be present for any compound to be an eiiicient antihistaminic agent, and that the antlhistaminic agents heretofore known attach to the receptor cells through or by means of one of these two groups.
It is the object of this invention to provide an entirely new class of antihistaminic agents.
Other objects of the invention will in part be obvious and in part appear hereinafter.
We have discovered that a new class of compounds having the general formula:
wherein R is an alkyl group containing from 1 to 4 carbon atoms, i. e. methyl, ethyl, propyl, and butyl and propyl and butyl isomers, and hydrohalide salts of such compounds are highly effective antihistazminic agents. The preferred antihistaminic compounds of our invention are 1-methyl-piperidyl-4-benzhydry1 ether and the hydrohalide salts thereof.
The compounds of our invention may be prepared by reacting a l-alkyli-piperidinol wherein the alkyl group contains from i to 4 carbon These new compounds may also be prepared by reacting l-alkyl-i-haloplperidines with benzhydrol or the sodium or potassium derivatives thereof or by reacting sodium or potassium derivatives of 1-alkyl-4-piperldinols with benzhydryl halides.
In preparing the compounds of our invention, the reaction may be carried out by heating the desired reactants together until the desired ether compound is formed. Preferably, the reaction is carried out in the presence of some inert solvent such as an aromatic or aliphatic hydrocarbon solvent or a high boiling aliphatic ether. Thus, for example, compounds such as benzene, toluene, xylene, heptane, octane, nonane, decane, dipropyl ether, dibutyl ether, diamyl ether, etc., may all be employed. The particular inert solvent which is used is not critical since its only function is to allow for a more emcient interaction of the reactants. Thus, any organic solvent such as those just mentioned which has a boiling point of about C. or above and which will not enter into reaction with either of the reactants being employed in preparing the desired compounds or with the desired compounds themselves may be used as a solvent in which to carry out the reaction. The amount of inert solvent, if any, which is employed is suitably equal to or slightly in excess of the amount of reactants being used. If desired, an excess of the l-alkyl-i-plperidinol compound may be employed to serve as a solvent medium for the reaction or, if desired, similar heterocyclic compounds such as pyridine, etc, may be utilized as a solvent medium tor the reaction. The reaction mixture may be heated under pressures greater than atmospheric if desired. Usually. it is preferred to heat the reaction mixture at the reflux temperature of the lowest boiling component thereof.
The two compounds which are to be reacted in each case to prepare one of the new compounds of our invention may be reacted in a mol to mol ratio or, if desired, an excess of the basic heterocyclic compound may be employed. If a mol to mol ratio of the reactants is used, the ether will be produced, at least to some extent, in the form of its hydrohalide salt. Preferably at least a molar excess of the basic heterocyclic compound is employed in carrying out the preparation of the compounds of our invention. One of the reasons for this is that .by having such an excess of a basic compound present any free hydrogen halide produced by the reaction will be neutralized by such excess basic compound and reaction mixture to neutralize any hydrogen halide which is formed.
The reaction should preferably be carried out under substantially anhydrous conditions in order to obtain the most favorable yields and therefore it is preferable to employ only substantially anhydrous reactants and solvents.
After the reaction medium has been heated for a suflicient length of time to give substantially complete reaction between the two reacting compounds, it will be found that the reaction mass will separate into two layers if an excess of a piperidinol or similar basic compound has been employed, the upper phase containing the desired benzhydryl ether compound. If an inert solvent such as xylene, toluene or one of the other;
aromatic or aliphatic hydrocarbon solvents has been employed, it will also be found in the upper phase. The lower phase of the reaction mixture will be made up of the excess piperidinol or similar basic compound, if any. If no inert solvent was utilized in the carrying out of the reaction, a volume of such a solvent equal to about the volume of the reaction mixture may be added thereto so as to aid in separating the desired benzhydryl ether compound from the rest of the reaction mixture. After separating the upper phase from the other components of the reaction mixture, if the reaction mixture has separated into two phases, any inert solvent in that phase is removed therefrom, e. g., by distillation under reduced pressure. The crude benzhydryl ether may then be purified by dissolving it in an excess of an aqueous acid solution of medium strength, e. g. 20% hydrochloric acid, and the aqueous acid solution then washed with some solvent such as ethyl ether to remove any non-basic impurities therefrom. If the reaction mixture does not separate into two phases, any inert solvent therein may be removed as by distillation under reduced pressure and the remainder of the reaction mix ture then admixed with an aqueous acid solution and the resulting mixture washed with a solvent such as ethyl ether to remove any nonbasic impurities. The aqueous acid solution of the desired benzhydryl ether compound may be decolorized with activated carbon and the acid solution neutralized with a base such as aqueous ammonia. The free benzhydryl ether compound will separate from the aqueous solution as an oily material and may be readily recovered by extraction with a solvent such as ethyl ether or a similar solvent. The oily product may then be converted to a crystalline hydrohalide salt by dissolving the oily product in a solvent such as isopropanol and adding thereto an alcoholic, e. g., methanolic, ethanolic, etc., halide. Ethyl ether may then be added to the acidified solution until a faint turbidity is observed. The crystalline hydrohalide salt of the benzhydryl ether will soon separate and after recovery from the solution may be further purified by recrystallization from a small amount of a solvent such as i-propanol if desired.
For a fuller understanding of the nature and objects of our invention, reference may be had to the following example which is given merely to illustrate theproduction of the compounds of our invention and such example is not to be construed in a limiting sense.
Example A mixture of 46 gm. of 1-methyl-4-piperidinol (0.4 mol), 49.4 gm. of benzhydryl bromide (0.2 moi) and 100 ml. of xylene was refluxed for approximately 24 hours. The reaction mixture separated into two phases with the upper phase containing the desired ether compound dissolved in xylene. The lower phase consisted of the hydrobromide salt of the excess i-methyli-piperidinol. The upper phase was separated from the lower phase and the desired benzhydryl ether recovered in the crude state by distilling of! the xylene under reduced pressure. The crude benzhydryl ether was a clear reddish oil. It was dissolved in '75 m1. of 20% hydrochloric acid and the aqueous acid solution then washed three times with 50 ml. portions each of ethyl ether. The aqueous acid solution was then decolorized with activated carbon and thereafter slowly admixed with '75 ml. of 28% aqueous ammonia. The benzhydryl ether separated as an oily material and was removed from the aqueous mixture by extraction with three 50 ml. portions of ethyl ether. On evaporation of the ethyl ether from the ethyl ether solution, the benzhydryl ether was recovered as a pale yellow oil. The benzhydryl ether was dissolved in 60 ml. of isopropanol and the isopropanol solution acidified to a pH of 3 with dry hydrogen chloride-methanol solution. The acidic propanol solution was then diluted with ethyl ether until a faint turbidity was observed. In a short time, the crystalline hydrochloride salt of the benzhydryl ether separated from the propanol solution. The crystallized salt was recrystallized once from 75 ml. of isopropanol with the aid of ethyl ether in order to further .purify the material. A yield of the pure hydrochloride salt of 1-methylpiperidyl-4-benzhydryl ether of 24.5 gm. was obtained. This was 39% of the theoretical yield. The pure material had a melting point of 206 C.
Calc. for C1sH24ONCl: C, 71.81; H, 7.61; N, 4.40; Ci, 11.15. Found: C, 71.25; H, 7.32; N, 4.07; C], 11.32.
The new compounds of our invention when tested physiologically have been found to have very good antihlstaminic properties with a very low order of undesirable side effects.
It will be noted that the chemical structure of our new antihistaminic agents is entirely different from the chemical structure of any of the previously known antihistaminic compounds. Thus it is quite apparent that we have provided an entirely new class of antihistaminic agents.
In addition to their antihistaminic properties, the compounds of our invention manifest antiasthmatic action when tested on animals.
Having described our invention, what we claim as new and desire to secure by Letters Patent is:
1. The class of compounds consisting of compounds having the structural formula wherein R is an alkyl group containing from 1 to 4 carbon atoms and the hydrohalide salts of such compounds.
2. The compound having the formula 8. The compound having the formula 4. The compound having the formula carbons and aliphatic ethers having boiling points of at least 80 C.. and the reaction mixture is heated at the reflux temperature of the inert solvent.
8. A process in accordance with the process of claim 6 wherein the reaction is carried out in the presence of an inert solvent selected from the class consisting of aliphatic and aromatic hydrocarbons and aliphatic ethers having boiling points of at least 80 C., and the reaction mixture is heated at the reflux temperature of the inert solvent.
LAWRENCE HOWLAND KNOX. ROLAND KAPP.
REFERENCES CITED The following references are of record in the file of this patent:
UNITED STATES PATENTS Number Name Date 657,880 Schmidt et al Sept. 11, 1900 2,369,611 Schening et al Feb. 13, 1945 2,453,729 Rievesahl Nov. 16, 1948 2,454,092 Rievesahl Nov. 16, 1948
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Cited By (10)

* Cited by examiner, † Cited by third party
Publication number Priority date Publication date Assignee Title
US2708194A (en) * 1952-12-10 1955-05-10 Univ Michigan 2-(1-methyl) polymethyleniminylmethyl benzhydryl ethers and preparation thereof
US2716122A (en) * 1953-10-19 1955-08-23 Nopco Chem Co N-substituted-4-benzhydryl ether-piperidines
US2745837A (en) * 1954-01-21 1956-05-15 Schering Corp Benzhydryl ethers of alkyl piperidinols
US2751388A (en) * 1950-04-07 1956-06-19 Nopco Chem Co Process for preparing benzhydryl ethers
US2784195A (en) * 1953-03-30 1957-03-05 Searle & Co Quaternary ammonium salts of nu-phenyl-nu-picolyl-dialkylaminoalkylamines
US2785173A (en) * 1953-03-17 1957-03-12 Searle & Co Dialkylaminoalkylphenetidinopyridine quaternary ammonium salts
US2831862A (en) * 1956-02-27 1958-04-22 Lakeside Lab Inc Ethers of n-alkyl-3-hydroxypiperidine and salts thereof
US2974146A (en) * 1956-02-24 1961-03-07 Lakeside Lab Inc 3-piperidyl benzhydryl ethers
US2991225A (en) * 1952-04-08 1961-07-04 Koninklijke Pharma Fab Nv Omicron-methylbenzhydryl-beta-dimethylaminoethyl ether process and composition for symptomatic relief of the syndrome of parkinsonism and of spastic skeletal muscle disorders
US20130324507A1 (en) * 2012-06-05 2013-12-05 Bioprojet Novel (aza)Benzhydryl Ether Derivatives, Their Process of Preparation and Their Use as H4-Receptor Ligands for Therapeutical Applications

Citations (4)

* Cited by examiner, † Cited by third party
Publication number Priority date Publication date Assignee Title
US657880A (en) * 1896-09-26 1900-09-11 Chem Fab Auf Actien Vormals E Schering Compound of vinyldiaceton-alkamins and process of making same.
US2369611A (en) * 1938-12-24 1945-02-13 Scheuing Georg Analgetically effective tetrahydronaphthalene piperidyl derivatives
US2453729A (en) * 1946-08-05 1948-11-16 Parke Davis & Co Benzhydryl amino ethers
US2454092A (en) * 1947-06-02 1948-11-16 Parke Davis & Co Benzhydryl amino ethers

Patent Citations (4)

* Cited by examiner, † Cited by third party
Publication number Priority date Publication date Assignee Title
US657880A (en) * 1896-09-26 1900-09-11 Chem Fab Auf Actien Vormals E Schering Compound of vinyldiaceton-alkamins and process of making same.
US2369611A (en) * 1938-12-24 1945-02-13 Scheuing Georg Analgetically effective tetrahydronaphthalene piperidyl derivatives
US2453729A (en) * 1946-08-05 1948-11-16 Parke Davis & Co Benzhydryl amino ethers
US2454092A (en) * 1947-06-02 1948-11-16 Parke Davis & Co Benzhydryl amino ethers

Cited By (11)

* Cited by examiner, † Cited by third party
Publication number Priority date Publication date Assignee Title
US2751388A (en) * 1950-04-07 1956-06-19 Nopco Chem Co Process for preparing benzhydryl ethers
US2991225A (en) * 1952-04-08 1961-07-04 Koninklijke Pharma Fab Nv Omicron-methylbenzhydryl-beta-dimethylaminoethyl ether process and composition for symptomatic relief of the syndrome of parkinsonism and of spastic skeletal muscle disorders
US2708194A (en) * 1952-12-10 1955-05-10 Univ Michigan 2-(1-methyl) polymethyleniminylmethyl benzhydryl ethers and preparation thereof
US2785173A (en) * 1953-03-17 1957-03-12 Searle & Co Dialkylaminoalkylphenetidinopyridine quaternary ammonium salts
US2784195A (en) * 1953-03-30 1957-03-05 Searle & Co Quaternary ammonium salts of nu-phenyl-nu-picolyl-dialkylaminoalkylamines
US2716122A (en) * 1953-10-19 1955-08-23 Nopco Chem Co N-substituted-4-benzhydryl ether-piperidines
US2745837A (en) * 1954-01-21 1956-05-15 Schering Corp Benzhydryl ethers of alkyl piperidinols
US2974146A (en) * 1956-02-24 1961-03-07 Lakeside Lab Inc 3-piperidyl benzhydryl ethers
US2831862A (en) * 1956-02-27 1958-04-22 Lakeside Lab Inc Ethers of n-alkyl-3-hydroxypiperidine and salts thereof
US20130324507A1 (en) * 2012-06-05 2013-12-05 Bioprojet Novel (aza)Benzhydryl Ether Derivatives, Their Process of Preparation and Their Use as H4-Receptor Ligands for Therapeutical Applications
US9242959B2 (en) * 2012-06-05 2016-01-26 Bioprojet (Aza)benzhydryl ether derivatives, their process of preparation and their use as H4-receptor ligands for therapeutical applications

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