US3265728A

US3265728A - Substituted phenethyl carbamates

Info

Publication number: US3265728A
Application number: US210818A
Authority: US
Inventors: Charles D Bossinger; Kelley G Taylor
Original assignee: Armour Pharmaceutical Co
Current assignee: Armour Pharmaceutical Co
Priority date: 1962-07-18
Filing date: 1962-07-18
Publication date: 1966-08-09
Anticipated expiration: 1983-08-09

Description

United States Patent SUBSTITUTED PHENETHYL CARBAMATES Charles D. Bossinger, Kankakee, and Kelley G. Taylor,

Decatur, lll., asslguors to Armour Pharmaceutical Company, Chicago, Ill., a corporation of Delaware No Drawing. Filed July 18, 1962, Ser. No. 210,818 12 Claims. (Cl. 260-482) This application is a continuation-impart of copending application Serial No. 729,554, filed April, 21, 1958, and of Serial No. 38,763, filed June 27, 1960, now abandoned. Application Serial No. 38,763 was a continuation-in-part of application Serial No. 729,553, filed April 21, 1958, now abandoned, and applications Serial Nos. 729,553 and 729,554 were continuations-in-part of parent application Serial No. 554,132, filed December 20, 1955, now abandoned.

This invention relates to certain substituted carbamate compounds and to a method of treating the central nervous system by administering these compounds. The novel compounds of this invention can be classified generally as substituted phenyl alkyl carbamate compounds.

It is an object of this invention to provide substituted phenyl carbamate compounds for use in treating the central nervous system which exhibit special and distinctive properties and/or combinations of properties, including tranquilization, sedation, and muscle relaxation. Further objects and advantages will be indicated in the following detailed specification.

The substituted phenyl carbamate compounds which are useful in the treatment of the central nervous system in accordance with the present invention are characterized by the following structural formula:

R: @t X R:

In the foregoing formula, R is either carbamate'or alkyl ylbenzyl, etc.

With respect to the above formula, one preferred subclass of compounds is obtained where R is carbamate, and R and R are hydrogen. These compounds are characterized by the structural formula:

' ii @om-c-c-mn Specific examples of compounds coming within the subclass represented by the above formula are: o-chlorobenzyl carbamate, 2,6-dichlorobenzyl carbamate, o-methylbenzyl carbamate, o-tri fiuoromethylbenzyl carbamate, pentachlorobenzyl carbamate, p-nitrobenzyl carbamate, m-nitrobenzyl carbamate, o-nitrobenzyl carbamate, 0-

. methoxybenzyl carbamate, m-methoxybenzyl carbamate,

p-methoxybenzyl carbamate, p-fiuorobenzyl carbamate,

' p-chlorobenzyl carbamate, 2,4-dichlorobenzyl carbamate,

m-chlorobenzyl carbamate, etc. 7

Again referring to the generic formula set out first above, another sub-class of compounds is obtained when R is methyl carbamate, R is hydroxy and R is hydrogen. These compounds are represented by the following structural formula:

ice

OH O

X Examples of compounds coming within this subclass are:

Referring again to the generic formula first set out above, still another sub-class of compounds is obtained when R is alkylene carbamate wherein the alkylene contains from 1 to 3 carbons, and R and R are hydrogen. These compounds are represented by the following structural formula:

Specific examples of compounds coming within this subclass are:

2- (p-chlorophenyl)-l-ethyl carbamate, 2-(o-chlorophenyl)-l-ethyl carbamate, 2-(2,4-dichlorophenyl)-l-ethyl carbamate, 2-(2,6-dichlorophenyl)-l-ethyl carbamate, 2-(p-rnethoxyphenyl)-1=ethyl carbamate, etc.

Still another subclass of compounds is obtained when R is carbamate, R is methyl, and R is hydrogen, referring again to the generic formula set out first above. These compounds can be represented by the following structural formula:

on, c @cH-o-c-NH, x

Specific examples of compounds coming within this subclass are: 1-(o-ch1orophenyl)-l-ethyl carbamate, 0:- methyl-p-phenylbenzyl carbamate, 2,6-dichloro-u-methylbenzyl carbamate, etc.

A preferred sub-class of compounds is obtained when R is alkylene carbamate, the alkylene containing from 1 to 3 carbon atoms, R is hydroxy, and R is alkyl containing from 1 to 3 carbons. These compounds are represented by the following structural formula:

X alkyl Specific examples of compounds coming within this subclass are:

2-(p-chlorophenyl)-2-hydroxy butyl carbamate, 2-(o-chlorophenyl)-2-hydroxy butyl carbamate, 2-(2,6-dichlorophenyl)-2-hydroxy butyl carbamate, 2-(o-methoxyphenyl)-2-hydroxy butyl carbamate,

Z-(p-bromophenyl)-2-hydroxy butyl carbamate,

2- (o-nitrobenzyl)-2-hydroxy butyl carbamate, 4-(p-chlorophenyl)-4-hydroxy hexyl-3-carbamate, and 2-(o-chlorophenyl)-4-hydroxy hexyl-3-carbamate.

A closely related group of compounds is obtained when hydrogen is substituted for the alkyl group in the formula last set out above. Specific examples of such compounds are:

Another sub-class of compounds is represented by the following structural formula:

0H (all: 0 @d-o-i'z-mn x I I Specific examples of such compounds are:

1-( p-bromophenyl)-2-hydroxyethy1 carbamate, 1 (p-chlorophenyl)-2-hydroxyethyl carbamate, l-(o-chlorophenyl)-2-hydroxyethyl carbamate, and 2-hydroxy-1-(o-methoxyphenyl)ethyl carbamate.

In all of the foregoing sub-generic formulas, the letter X has the same meaning ascribed to it in the generic formula set out first above. It will be further understood that X is not limited to a single substituent group, as illustrated by many of the foregoing specific compounds.

Many if not all of the foregoing compounds can be prepared by the process described in copending application Serial No. 161,739, filed December 22, 1961, now abancloned. In that process the first step is the preparation of an organic cyclic carbonate from which the desired carbamate compound can be obtained. The cyclic carbonate can be made by dissolving a substituted phenyl ethane diol in a dialkyl carbonate and heating this reaction mixture to evaporate the hydroxy alkyl reaction by-product. This leaves the organic cyclic carbonate reaction product as the residue. If desired, an alkali catalyst may be used. The cyclic intermediate is a substituted 4-phenyl ethylene carbonate, which is preferably reacted with ammonia to split the carbonate ring and form the desired carbamate. This procedure is described in greater detail in the cited application Serial No. 161,739.

Other processes can be used to prepare the substituted phenyl carbamates. In one such procedure, a 1,2-glycol is converted to the corresponding carbonate, and the carbonate is subjected to an ammonolysis to obtain the desired carbamate. This process was described in prior application Serial No. 816,700, filed May 29, 1959, now U. S. Patent No. 3,066,164. Preferably, a 1,2-glyco1 is condensed with a halo-formic ester to obtain an acyclic carbonate which is then subjected to ammonolysis to obtain the monocarbamate. Since the particular process for preparing the carbamate compounds does not form a part of the present invention, it is not believed it will be necessary to further describe such processes herein, except that the preparation of specific carbamate compounds will be subsequently illustrated.

In utilizing the compounds of this invention for central nervous system treatment it is preferred to administer the compounds orally. Since the compounds are well-absorbed orally, it will usually not be necessary to resort to parenteral administration. For oral administration, it is preferred to combine the carbamate compound with a pharmaceutical carrier. The proportions of the carrier and carbamate compound are not critical, and they vary considerably depending whether the composition is to be filled into capsules or formed into tablets. In tableting, it will usually be desirable to employ at least as much of the pharmaceutical carrier as the carbamate compound. Various edible pharmaceutical carriers, or mixtures thereof can be used. For example, a mixture of lactose, dibasic calcium phosphate, and cornstarch is suitable. Additional ingredients can be included, such as lubricants like magnesium stearate.

When administering the compounds of this invention orally for central nervous system treatment, the total daily dose will usually fall within the range from 400 to 2000 milligrams of the carbamate compound per 24 hour period. Typically, the daily dose will range from 600 to 1600 milligrams. In some cases, it may sometimes be desirable to administer as much as 2400 milligrams per day. In practicing the method of this invention, it will therefore be convenient to have the carbamate compound combined with a pharmaceutical carrier and prepared in tablets or other dosage unit form. Each tablet or dosage unit can contain from 50 to 600 milligrams of the carbamate compound. For example, tablets containing 200 milligrams of the carbamate compound can be administered either 1 tablet three times a day to achieve a daily dose of 600 milligrams or up to 2 tablets four times a day to achieve a daily dose of 1600 milligrams.

The present invention is further illustrated by the following specific examples.

Example I l-(p-chlorophenyl)-l,2-butanediol 20 g. (0.1 mole), diethyl carbonate 12.1 ml. (0.1 mole), and potassium carbonate 0.1 g. were mixed in a round-bottomed flask fitted with a Vigreux column. The reaction mixture was heated with an oil bath at approximately 150 C. The ethanol which was formed during the reaction was distilled. After the theoretical amount of ethanol was removed, the diethyl carbonate, if any, was distilled under reduced pres sure.

The residue, when cooled to room temperature, was put into 300 ml. of methanol saturated with ammonia at 0 C. Occasional shaking was necessary to facilitate solution. The reaction mixture was left standing at room temperature overnight. The ammoniacal solution was filtered and the filtrate was contrated under reduced pressure. The product was dried by azeotropic distillation with benzene. After benzene was removed, a slightly yellow semisolid was obtained. It was triturated with CC], to give a White solid, 9.3 g. The solid was recrystallized twice from CC], to crystals, 6.2 g. of l-(p-chlorophenyl)-1-hydroxy-2-butyl carbamate.

Example 2 2-(p-biphenyl)-1,Z-butanediol 24.2 g. (0.1 mole), diethyl carbonate 12.1 ml. (0.1 mole), and potassium carbonate 0.1 g. were mixed in a round-bottomed flask fitted with a Vigreux column. The reaction mixture was heated with an oil bath at approximately 150 C. The ethanol which was formed during the reaction was distilled. After the theoretical amount of ethanol was removed, the diethyl carbamate, if any, was distilled under reduced pressure.

The residue, when cooled to room temperature, was put into 300 ml. of methanol saturated with ammonia at 0 C. Occasional shaking was necessary to facilitate solution. The reaction mixture was left standing at room temperature overnight. The ammoniacal solution was filtered and the filtrate was concentrated under reduced pressure. The product was dried by azeotropic distillation with benzene. After benzene was removed, a yellow semi-solid was obtained. It was triturated with benzene to give a solid, 13.6 g. It was twice recrystallized to give crystals 10.5 g. of 2-(p-biphenyl)-2-hydroxybutyl carbamate.

Example 3 night.

v benzyl carbamate.

This solid was placed in 250 ml. of anhydrous methanol saturated with ammonia in the cold; Occasional shaking was necessary to facilitate solution. The reaction mixture was left standing over night.

The methanolic solution was filtered and concentrated under reduced pressure. A solid residue was obtained. It was washed with 4% NaOH thoroughly several times, filtered, and air dried. The crude product, 10.1 g., was recrystallized from benzene twice and then ethyl acetate, to give white crystals 2.5 g., M.P. 179l80.5 of amethyl-p-phenylbenzyl carbamate.

Example 4 that water was driven off with toluene as an azeotrope. I The reaction mixture was left to cool slightly. Aluminum isopropylate, 0.75 g. was then added. The oil bath was kept at 14S-155. An azeotropic mixture of tolueneand I ethanol was distilled. Distillation was stopped when the head temperature dropped to 55".

After toluene was removed under reduced pressure, a

solid residue was obtained. It was dissolved in a minimum amount of hot chloroform and filtered off any insoluble material. After the filtrate was cooled down to room temperature, white needles formed and isolated by suction filtration; It was recrystallized from benzene to give needles, l2.3g., M.P. 160.5-l62.5, yield 35.0%,

of 2-(2,6 dichlorophenyl)ethyl earbamate.

Example 5 To 17.8 g. of ethyl carbamate (0.2 mole) in a roundbottomed flask fitted with a distillation setup were added 24.4 g. of o-methylbenzyl alcohol (0.2 mole) and] 1.00 ml. of toluene. The system was heated so that water was driven off with toluene as an azeotrope. The reaction mixture was left to cool slightly. Aluminum isopropylate, 1.0 g., was then added. The oil'bath was kept at 145- 155. An azeotropic mixture of toluene and ethanol was distilled. Distillation was stopped when the head temperature dropped to 55.

After toluene was removed under reduced pressure, a solid residue was obtained. It was dissolved in hot chloroform and filtered off any insoluble material. The filtrate was concentrated under reduced pressure leaving a solid residue. It was recrystallized from carbon tetrachloride three times to give crystals, 12.6 g., M.P. 88-90, yield 38.1%, of o-methy'lbenzyl carbamate.

Example 6 To 17.8 g. of ethyl carbamate (0.2 mole) in a roundbottomed flask fitted with a distillation setup were added 28.5 g. of o-chlorobenzyl alcohol (0.2 mole) and 75 ml. of toluene. The system was heated so that water was driven off with toluene as an azeotrope. The reaction mixture was left to cool slightly. Aluminum isopropyl ate, 1.5 g., was then added. The oil bath was kept at 145-155. An azeotropic mixture of toluene and ethanol was distilled. Distillation was stopped when the head temperature dropped to 55.

After toluene was removed under reduced pressure, a slightly yellow solid residue was obtained. The residue 7 Example 7 A p-Brornostyrene glycol 22 g. (0.1 mole) and 200 ml ofwbenzene were placed in a three-necked fiask equipped in the usual manner. While stirring, 18 g, of phosgene in ml. ofbenzcnc was added slowly in approximately 10 minutes. After an additional 50 minutes of stirring, 18 g. of diethyl aniline in 50 ml. of benzene was added. The reaction became exothermic when half of the diethylaniline wasadded. A cold water bath was used during the rest of the addition.

After an hour of stirring, the benzene solution was washed once with 250 ml. of cold water. It was then added to 180 ml. of 30% NH OH-in the cold. The reaction mixture was stirred for two hours. A white solid was isolated by filtration and air dried. The product weighed 18.5 g. and had a melting range, of 68-140 (I). Ali tel" standing for three days, a second crop of solid (II) was isolated from the water-benzene filtrate. (II) weighed 3.6 g., M.P. 158-161. It was recrystallized from chloroform to give crystals 3.18 g., M.P. 162-'-164 of Z-(p-bromophenyl)-2-hydroxy-1-ethyl carbamate.

(I) was dissolved in hot water, filtered, allowed to cool, and left standing for five hours. An oil precipitated out and solidified on standing The solid (III) was isolated by filtration. lt weighed 9.4 g., M.P. 86-123". (III) was dissolved in CHCI A fter chilling in an ice bath. a powdery material, 2.16 g., M.P. 154459", was obtained. The filtrate was concentrated to -a volume of ml. After chilling in an ice bath, crystals (IV) 4.12 g., M.P. 7073, were isolated. (IV) was dissolved in 450 ml. of benzene on the steam bath. After standing at room temperature overnight, clusters of crystals, l-(p-br0m0- phenyl)-2-hydroxy-l-ethyl ca-rbamate 1.4 g., M.P. 99- 101", was obtained.

Example 8 Tablets for oral administration can be prepared from o-chlorobenzyl carbamate as follows: The compound is combined wit-h a. mixed pharmaceutical carrier in the ratio of 2 parts by weight of the carbamate compound per 3 parts of the pharmaceutical carrier. The mixed carrier contains dibasic calcium phosphate as the principal ingredient together with smaller amourts of lactose and 1 part of cornstarch. A small amount f magnesium stearate is also included.

The carbamate compound, the calcium phosphate, the lactose, and part of the magnesium stearate are blended and dry mixed until a uniform composition was obtained. This is formed into firm slugs no greater than A inch thick. The slugs are then put through an oscillating granulator equipped with a 10 mesh screen. The cornstarch and a little more magnesium stearate is added at intervals while the slugs were being sized. The granulation is blended in a drum tumbler for 30 minutes. Following this, the granulation is compressed into tablets of 500 mg. per tablet containing 200 milligrams ofv the carbamate compound. This preparation acts on the central nervous system and lowers body temperature.

While in the foregoing specification, this invention has been described in relation to certain preferred embodiments, and many details have been set forth for purpose of illustration, it will be apparent to those skilled in the art that the invention is susceptible to additional embodiments, and that certain of the details set forth herein can be varied considerably without departing from the basic principles of the invention.

We claim:

1. Substituted phcnyl alkyl ca-rbamate compounds having the structural formula wherein R selected froin the class consisting of carbamate and methylene carbamate, R is selected from the class consisting of alkyl containing from 1 to 2 carbons, hydroxy alkyl containing from 1 to 2 carbons, hydroxy, and hydrogen, and R is selected from the class consisting of hydrogen and alkyl containing from 1 to 2 carbons, and X is selected from the class consisting of halogen, methyl, methoxy, phenyl, n-itro, and amino.

2. The carbamate compounds of claim 1 wherein R is carbamate, and R and R are hydrogen.

3. The carbamate compounds of claim 1 wherein R is cnrbumzite, R is hydroxy-methyl, and R is hydrogen.

4. The carbamate compounds of claim 1 wherein R is methylene cnrbamate, R is hydroxy, and R is alkyl containing 1 to 2 carbons.

5. Substituted phenyl alkyl carbamates having the structure I ll @cnwm-o-o-mn 8 9. 2-(alkoxyphenyl)-2-hyd roxyethyl ca'rbamate wherein said alkoxy is a lower alkoxy.

10. 2-(chlorophenyl)-2-hydroxyethyl carbamate. 11. 2-(bromophenyl)-2-hydroxyethyl carbamate. 12. 2-(alkylphenyl)-2-hydroxyethyl carbamate where in said alkyl is a lower alkyl.

References Cited by the Examiner UNITED STATES PATENTS 2,197,479 4/1940 Meigs 260-482 2,627,524 2/1953 Mnlkemus 260--4S2 2,878,158 3/1959 Stuehmer 260-482 2,890,984 6/1959 Sahyun 167-65 2,967,880 1/1961 Finke 260482 3,036,954 5/1962 Robbins 16765 FOREIGN PATENTS 230,632 10/1958 Australia.

1,132,914 7/1962 Germany.

OTHER REFERENCES Mills, Proc. Soc. Exp. Biol. Med., vol. 96, pp. 100102 (1957).

LORRAINE E. WEINBERGER, Primary Emminer. M. O. WOLK, LEON ZITV'ER, Examiners.

P. SABATI NE, D. P. CLARKE, R. K. JACKSON,

Assistant Examiners.

Claims

1. SUBTITUTED PHENYL ALKYL CARBAMATE COMPOUNDS HAVING THE STRUCTURAL FORMULA