CH314569A - Process for the preparation of an anesthetic - Google Patents

Description

  

  Process for the preparation of an anesthetic Esters of carbanilic acid derived from amino alcohols with alkyl or alkoxy groups in the 2,6- or 2,4,6-position of the phenyl radical have excellent anesthetic properties, such as high effectiveness, low toxicity and good stability of their solutions Salts, which makes them suitable for both surface and injection anesthesia.

   A decisive factor for the effectiveness and stability of these esters is the symmetrical arrangement of the substituents in the phenyl nucleus of the carbanilic acid, and studies have shown that especially the carbanilic acid esters of alcohols of the type of piperidinoalkanols and dialkylaminoalkanols have favorable properties point.

      The compounds correspond to the formula
EMI0001.0022
    in which R1 and% are alkyl or alkoxy groups, R. is hydrogen, alkyl or an alkoxy group, R4 is a branched or urebranched, saturated or unsaturated hydrocarbon chain with a maximum of 6 carbon atoms and R ,,

      and R6 denote alkyl groups or together with the nitrogen denote a saturated heterocyclic ring.



  These anesthetics can be made as follows: An aryl isoeyanate of the formula
EMI0001.0041
    is first at room temperature and then at elevated temperature with an amino alcohol of the formula
EMI0001.0045
    implemented. The amino alcohol can also be used in the form of a salt.



  The reaction starts spontaneously when equivalent amounts of the two components are brought together. Since it is extremely exothermic, you should cool and preferably work in an inert solvent. In order to bring the reaction to the end, it should be heated to about 100 C for another 1-2 hours. The reaction product, the substituted carbanilic acid aminoalkyl ester, can be easily. isolate if a solvent was used, e.g.

   B. by extraction with dilute hydrochloric acid. The hydrochloric acid solution can then be cleaned with activated charcoal and sodium dithionite after adjusting the pH of the solution to 6.5. The base can then be obtained by precipitation with ammonia.



  The present patent now relates to a process for the preparation of 2,6-dimethyl-carbanilic acid-ss-piperidino-ethyl ester, which is characterized in that 2,6-dimethyl-phenyl-isocyanate is used with s-piperidino-ethy. converts alcohol.



  A salt of this base can also be used in place of the piperidino-ethyl alcohol. _ <I> Example </I> To a solution of 147 parts of 2,6-dimethylphenyl isocyanate in 200 parts of benzene, 129 parts of β-piperidino-ethyl alcohol are added with stirring and cooling. After everything has been added at about 50 C and the reaction has subsided, the solution is heated to boiling under reflux for 2 hours, whereupon the 2 formed

  6-Dimethylcarbanilsänre-s-piperidino-ethyl ester extracted with dilute hydrochloric acid. After adjusting the pH to about 6.5, the hydrochloric acid solution is treated with 20 parts of activated charcoal and 1 part of sodium dithionite. If carefully precipitated with ammonia, the free ester is obtained as a white, crystalline precipitate. It melts at 80-82 C.



  The hydrochloride is a white crystal powder with a melting point between 167 and 169 C.

 

Claims (1)

PATENT CLAIM Process for the production of 2,6-dimethyl-carbanilic acid-ss-piperidino-ethyl ester, characterized in that 2,6-dimethyl-phenyl-isocyanate is reacted with β-piperidino-ethyl alcohol. The compound obtained is a white crystalline solid with a melting point of 80-81 ° C, which forms a white hydrochloride with a melting point of 167-169 ° C. SUBClaims 1. The method according to claim, characterized in that one works first with cooling and then with heating to about 100 C. 2. Method according to claim, characterized in that one works in the presence of an inert solvent.