DE1005970B - Process for the production of new hydrazones of the 5-nitrofuran series - Google Patents

Description

Process for the Production of New Hydrazones of the 5-Nitrofuran Series This invention relates to the production of new chemical compounds which exert a high therapeutic effect against microbial infections in vivo and which are very well tolerated by the organism when administered orally. They own the general formula in which X represents sulfur or an imino or methylene group.

The members of this class of compounds are distinguished by the fact that they are effective against infections despite surprisingly low toxicity, which caused by both gram-positive and gram-negative microorganisms. They have when taken perorally in sub-toxic, appropriately divided doses with pathogenic organisms, e.g. B. Salmonella typhosa, fatally infected animals applied after infection are more effective than the compounds available in U.S. Patent 2,610,181. The percentage of surviving animals was only 20 0% here, in the case of the compounds according to the invention on the other hand 65 to 95%. So they are extremely effective chemotherapeutic agents before. The new compounds have both healing and prophylactic effects on microbial ones Infections. You can therefore not only in high single doses to an acute one To counter seizure, be administered, but also in small, subliminal Doses to prevent infection in the first place. The oral Administration can be in the form of tablets, capsules, powders and suspensions take place. The new compounds can also be used as prophylactic agents in veterinary medicine can be used, being expediently added to the feed or drinking water.

We have discovered that the members of our new series of compounds are obtained in good yield by reacting 5-nitrofurfurol or its diacylates with the amino compounds of the corresponding heterocyclic compounds, ie imidazolidones, pyrrolidones and thiazolidones, preferably in the presence of an inert, acid-containing solvent such as can be seen in detail from the following examples. In the context of the present application, no protection is sought for the manufacturing processes for the starting materials mentioned in these examples. Example 1 N- (5-Nitro-2-furfurylidene) -1-amino-2-imidazolidone A. N-Carbethoxy-N- (2-benzalaminoethyl) -N'-benzalhydrazone.

146 g (0.57 mol) of 2-aminoethylhydrazine-dioxalate are moistened with water, whereupon a solution of permanent basicity is produced by adding 15% sodium hydroxide solution. The mixture is cooled well and the precipitated sodium oxalate is filtered off; the filter cake is washed out well with cold water. The clear, aqueous filtrate is heated to 55 ° and treated with 130 cc (1.3 mol) of benzaldehyde. The mixture is stirred for about 15 minutes and kept at a pH of about 8 by adding the necessary amount of sodium hydroxide. The reaction mixture is then cooled and extracted completely with ether. After removal of the ether, a syrupy residue of N- (2-benzalaminoethyl) -N'-benzalhydrazone, C, Hb-CH = N-CHz-CH, -NH-N = CH-CBHs, remains. This residue is dissolved in 300 cc of alcohol dissolved and treated in the course of about 35 minutes with 57 ccm (0.6 mol) of ethyl chlorocarbonate at 15 to 25 °. During the reaction, the p $ is kept at about 7 to 7.5 by adding 150% strength sodium hydroxide solution. Stirring is then continued for an hour. The product is filtered off, washed with water and air-dried. Yield 107g (580/0). This material is pure enough for the next reaction. It can be purified by recrystallization from alcohol and then melts at 105 to 105.5 °. Formula: B. ethyl 1- (2-aminoethyl) carbazate [= N-amino-N- (2-aminoethyl) carbamic acid ethyl ester]. 300 cc of 10% sulfuric acid are added to 107 g (0.33 mol) of the crude N-carbethoxy-N- (2-benzalaminoethyl) -N'-benzalhydrazone and the mixture is subjected to steam distillation until no more benzaldehyde passes over. The aqueous solution is then treated with animal charcoal and filtered. A slight 1st excess is then added to the barium hydroxide solution; the precipitated barium sulfate is filtered off and washed well with water. The aqueous filtrate is distilled largely anhydrous in vacuo and the residue is taken up in methanol. The solution is filtered and the residue is washed well with methanol. The methanolic solution is evaporated and the residue is freed from water by azeotropic distillation with benzene. The product obtained satisfies the requirements for the next reaction. It can be purified by vacuum distillation. The pure carbamic acid ester boils at 131 to 131.5 ° / 2mm. Formula: C. 1-Amino-2-imidazolidone.

The crude carbamic acid ester as obtained above is used added to a solution of 1.6 g (0.07 mol) of sodium in 25 cc of methanol. The mixture is heated with stirring for 40 minutes, the temperature increasing from 103 to 120 ° will. During this time, 33.5 cc of distillate go over from 65 to 72 °. The residue, consisting essentially of crude 1-amino-2-imidazolidone, can be used directly for manufacture of N- (5-nitro-2-furfurylidene) -1-amino-2-imidazolidone can be used, or he can be cleaned by distillation at 2 mm and 200 °. The distilled material After recrystallization from alcohol, it melts at 111.5 to 112 ° and is pure 1-amino-2-imidazolidone. D. N- (5-nitro-2-furfurylidene) -1-amino-_ 2-imidazolidone. The crude 1-amino-2-imidazolidone is dissolved in water, which is acidified with hydrochloric acid and treated with a solution of 40 g of 5-nitro-furfural in alcohol. You get so 34 g of N- (5-nitro-2-furfurylidene) -1-amino-2-imidazolidone with a melting point of 253 to 260 ° (with decomposition), that is 46 °%, based on the N-carbethoxy-N- (2-benzalaminoethyl) -N'-benzalhydrazone used. Recrystallization from nitromethane using animal charcoal gives the pure compound that melts at 261.5 to 263 °.

In compliance with the procedure described in 1 D are in place _der- 40 g of 5-nitrofurfural 69 g of 5-nitro-2-furfural diacetate., used. On it will the reaction mixture heated briefly to 80 to 90 °, the same yield of the desired end product is obtained.

Example 2 N- (5-nitro-2-furfurylidene) -1-amino-2-pyrrolidone A solution of 107 g (1.26 mol) of 2-pyrrolidone in 650 ccm of 2N hydrochloric acid is cooled to -3 °, and 91.3 g (1.26 mol) of sodium nitrate are added over the course of 2 hours, in such a way that the Temperature does not exceed 0 °; the solution is then stirred for a further hour while cooling with ice. Sodium chloride is then added to saturation and extracted exhaustively with ether. The ether is distilled off and the residue is dried in vacuo; Yield 106 g (740/0) of N-nitrosopyrrolidone- (2) as a yellow oil.

The nitroso compound thus obtained becomes electrolytic on a mercury cathode reduced by 9 cm 0; 2 lead anodes in porous cylinders are used as the anode and 100% sulfuric acid used as the electrolyte. A current density of 0.158 amps / cm2 is obtained by using a current of 10 Amp. and the temperature holds on - 5 to 0 °. To reduce 53 g (0.465 moles) of the nitroso compound are theoretically 5 hours necessary. After 3 hours, bubbles escape, and at the end of the 5th The solution is colorless for hours. To remove about 3 g of yellow oil, the Reaction mixture extracted with ether. The purified aqueous solution is with a Solution of 23 g of 5-nitro-2-furfurylaldehyde in alcohol and put in overnight Left the icebox. The product is filtered off, washed with alcohol and ether and dried; Yield 33.8 g (32.5 ° / °) from melting point 228 to 230 °. By Recrystallization from a nitromethane-alcohol mixture (1: 2) increases the melting point to 233 to 233.5 °. The compound must be kept in the dark as it is exposed to light gets dark quickly.

The procedure described in Example 2 is followed, with the exception that instead of the 23 g of 5-nitrofurfural 39.6 g of 5-nitro-2-furfural diacetate be used. The mixture is briefly heated to 80 to 90 °, the same Yield of the desired end product is obtained.

Example 3 N- (5-Nitro-2-furfuryhden) -3-amino-2-thiazolidone A mixture of 248 g (2.2 mol) of 2-aminoethyl mercaptan hydrochloride and 264 g (4.4 mol) of urea are heated to 170 to 180 ° in an oil bath, then to 200 ° for 30 minutes until the ammonia development has become very low. The cooled mixture is stirred with ethyl alcohol; the ammonium chloride is filtered off and washed thoroughly with alcohol. The oil remaining after the alcohol has been distilled off is treated with dioxane; the deposited solid product is filtered off and washed thoroughly with dioxane. The dioxane is distilled off and the residue is distilled in vacuo; Yield 134 to 140 g (600%) of crude 2-thiazolidone with a boiling point of 142 to 150 ° at 3.5 to 4.5 mm (126 to 127.5 ° at 1.7 mm); the melting point is 36 to 46 °. The crude product can be purified by recrystallization from carbon disulfide, the melting point increasing to 50 to 52 °.

A solution of 34.7 g (0.34 mol) of the crude 2-thiazolidone in 110 ccm 10% hydrochloric acid is cooled to 0 ° and in the course of approximately 15 minutes with a solution of 23.3 g (0.34 mol) of sodium nitrite in 70 cc of water at 0 to 4 ° treated. When the addition is complete, the mixture is cooled with ice for 30 minutes stirred and the solid nitroso compound filtered off and washed with ice water. The substance can be further processed directly.

The raw, moist nitroso compound becomes electrolytic on a mercury cathode reduced; there is a lead anode in the clay cylinder and 10% sulfuric acid Electrolyte used. A current density of 0.159 amps / cm2 is used with one Temperature from -2 ° to -E- 2 °. The reduction is carried out for 3 hours and 10 minutes, that is 30 minutes longer than the theoretically required time. After the reduction the aqueous solution is extracted with ether to remove some oily impurities remove, and then with an alcoholic solution of 25 g of 5-nitro-furfural treated. After cooling overnight, the yellow product is filtered off and washed with alcohol-ether washed. Yield 37.5 g (46%) with a melting point of 224 to 226 °. Recrystallization from a 1: 1 nitromethane-alcohol mixture improves the melting point to 226.5 up to 227 °.

The procedure described in the previous example is carried out with the Change retained, that instead of 25 g of 5-nitro-2-furfuro, 143 g of 5-nitro-2-furfural diacetate can be used for condensation. It is heated briefly to 80 to 90 °. You get the same yield of the desired end product.

Claims (1)

PATENT CLAIM: Process for the production of new hydrazones of the 5-nitrofuran series of the general formula in which X is -S-, - NH - or -CH, - , characterized in that 5-nitrofurfurol or its diacylates are mixed with amines of the general formula preferably condensed in the presence of an inert, acid-containing solvent. Referred to U.S. Patent No. 2,610,181.