FI59587B - NYTT FOERFARANDE FOER FRAMSTAELLNING AV PIPERAZINDERIVAT - Google Patents

Description

r ,, .... ADVERTISEMENT ¢ -0507 VST * M <11> utlKogninosskrift 5 »00 / C (45) Patent granted 10 09 1931 .tfiÄjöj Patent rceddelat vvy (51) Kv.ik.Wci.3 c 07 D 295 / 16 FINLAND —FINLAND (M) htM «MiMM-PmnMieknlii | 793712 (22) KUkcmtapilvI — AiN & knlngadaf 27.11.79 (Fl) (23) AlkupUv · —Glltlfhattdtf 15.06.72 (41) Tullut JulklMkil — Uhrit 0 # T * mH | 11/27/79

Htwtttl- and r ^ imrlWIItu. 0 "

Pmtant- och mlUtritynlun AnaMan utfafd od) utl- * k «1ft * n publicurad 29.05.Oi (32) (33) (31)« tty ueiollwu · —toflrt priority (71) Delalande SA, 32 rue Henri Regnault, Courbevoie (Hauts -de-Seine),

France-France (FR) (72) Gerard Huguet, Le Pinson Malesherbes (Loiret), Claude Fauran, Paris,

Guy Raynaud, Paris, Bernard Pourrias, Meudon La Foret (Hauts-de-Seine), Michel Turin, Paris, France-France (FR) (7 * 0 Leitzinger Oy (5 * 0 New method for the preparation of a piperazine derivative) The present invention relates to a new process for the preparation of a compound of formula I.

H3CO

h3co —CH = CH "C0" _ / NH U> H3CO

The compounds of formula I prepared according to the invention are useful in the preparation of pharmaceutically valuable piperazine derivatives of formula

H3CO

H3CO-O CH = CH - CO - ^ - CH2 - CO R (II>

H3CO

2,59587 The preparation of these compounds has been described e.g. in "Chimie Therapeutique", No. 4, pages 290-292 (1969), according to which substituted piperazine is reacted with 3,4,5 trimethoxycinnamoyl acid halide. The starting materials used in such a process are difficult to prepare, so the cost of the compound to be prepared is quite high. Another disadvantage is that the chain of reagents is cleaved in the reaction and this cleaved chain is attached to the unsubstituted nitrogen atom of the starting piperazine to give a disubstituted piperazine as a by-product.

It has now surprisingly been found that a compound of formula I can be prepared in a simple manner with virtually no undesired by-products by reacting 1- (3,4,5-trimethoxycinnamoyl) -4-formylpiperazine with aqueous hydrochloric acid. The starting materials used in the invention are all readily available commercially. In addition, the process can be completed in a simple manner and the side reactions do not interfere with the course of the reaction.

The following is an example of the application of the method according to the invention.

Example (3,4,5-trimethoxycinnamoyl) piperazine

To a solution of 512 g (2 moles) of 3,4,5-trimethoxy-cinnamic acid chloride in 4 liters of chloroform containing 252 g (3 moles) of sodium bicarbonate is added 228 g (2 moles) of formylpiperazine within one hour, and the mixture is allowed to react. cold for 6 hours. The solution is then filtered and the filtrate is concentrated. After recrystallization from absolute alcohol, 424 g of 1- (3,4,5-trimethoxycinnamoyl) -4-formylpiperazine are obtained.

Melting point 134 ° C Yield 63% 3,59587 At 90 [deg.] C., a suspension of 0.32 mol (106 g) of 1- (3,4,5-trimethoxycinnamoyl) -4-formylpiperazine is added over 6 hours to 320 ml. 10% aqueous hydrogen chloride solution.

The resulting solution is concentrated. After recrystallization from absolute alcohol, 70% of 3,4,5-trimethoxycinnamoylpiperazine hydrochloride is obtained.

Melting point 192 ° C Yield 64% f i i i