DE1110633B - Process for the production of vitamin A acid nitrile or esters - Google Patents

Description

Process for the production of vitamin A2 acid nitrile or esters It is known that vitamin A2 acid esters can be prepared by using N-bromosuccinimide bromine in the cyclohexene ring of the vitamin-Al-acid methyl ester a-position introduces to the double bond and then with the help of a base hydrogen bromide split off with formation of the cyclohexadiene ring (K. R. Farrar and co-workers, J. Chem. Soc.

[London], 1952, p. 2657). The procedure, however, continues over several Staged synthesis of the vitamin Al acid ester precedes and thus loses of technical interest.

It has now been found that vitamin A2-acid nitrile or ester can be produced in a simple manner and in good yields if B-dehydrojonylidene acetaldehyde is used with isolated, resonance-stabilized triphenylphosphine methylenes, ie phosphorylenes with strongly electron-attractive groups of the general formula where R denotes a cyano, carbalkoxy, carbocycloalkoxy or carbaryloxy radical, is reacted in a strongly polar solvent at elevated temperature, optionally in the presence of antioxidants and with the exclusion of oxygen. The reaction can be illustrated by the following equation: It is known from the German Auslegeschrift 1026 745 to condense the ß-Jonylidenacetaldehyd with a phosphorylene of the general formula, in which R denotes the carbomethoxy radical to the vitamin A-acid methyl ester in such a way that you first the phosphorylene from the corresponding phosphonium salt with With the help of strong proton acceptors, such as sodium acetylide or sodium amide, and then adding the aldehyde component without isolation. However, this procedure has - transferred to the production of vitamin A2 derivatives - the disadvantage that the proton acceptor, even if it is used in deficit, does not react completely with the phosphonium salt due to its poor solubility in the solvent used and when it is added of the ß-dehydrojonylidenacetaldehyde of the formula II gives rise to self-condensations of the aldehyde, which become the main reaction when the batch is heated even in the presence of an antioxidant and polymerization retarder such as phenothiazine or hydroquinone. This forces you to use an excess of aldehyde. However, this is uneconomical since the aldehyde is the most valuable component of the reaction. In addition, you have to work at room temperature and thus accept long reaction times.

On the other hand, strongly resonance-stabilized ones react under these conditions Phosphinmethylenes of the type of compound I in which the radical R is about a cyano group means, only in very poor yield with the ß-Dçhydrojonylidenacetaldehyd.

The inventive method avoids these disadvantages by first the phosphorylenes, which are stable to water and atmospheric oxygen at room temperature isolated and then subsequently with the aldehyde in a strongly polar solvent implements. This procedure gives the products of the invention Process in high yield.

Cis- and trans-13-dehydrojonylidene acetaldehydes are suitable for the process according to the invention and mixtures thereof. They are obtained from the corresponding alkyl B-dehydro3onylideneacetates, in that in the first stage of the process the esters mentioned are known per se Way with complex metal hydride complex compounds, such as lithium aluminum hydride, reduced and in the second stage of the process the ß-dehydrojonylidenethanols obtained dehydrogenated in a manner known per se with manganese dioxide to give the corresponding aldehyde.

The phosphorylenes suitable for the present invention of the general Formula I is produced from the corresponding phosphonium salts by treatment their z. B. aqueous solutions with excess dilute aqueous alkali, e.g. B. Soda or potassium hydroxide solution at 5 to 100 C.

Strongly polar solvents are particularly suitable as solvents, which do not react with the starting materials even when heated, e.g. B. acetonitrile, Dimethyl sulfone, tetramethylene sulfone or tetrafethyl urea. You can do without further mixtures of these solvents with one another or with non-polar or weakly polar solvents, such as petroleum ether, benzene, xylene or ether, with advantage use. The mixing ratio can and will fluctuate within wide limits determined by the reaction temperature required for the particular batch.

Expediently, 1 mol of the aldehyde is used with exclusion of moisture with 1 to 1.5 moles of the phosphorylene, preferably with 1.1 moles between 50 and 2000 C, preferably between 60 and 1000 C, to. The reaction time depends on the structure of the phosphorylene used and the reaction temperature and is between 30 minutes and 4 hours. It is best to use an antioxidant, e.g. B. Phenothiazine, add and work with the exclusion of water and oxygen.

Working up can be carried out by known methods and is preferably made by pouring the mixture into 100% phosphoric acid and Ice and subsequent absorption of the reaction product in petroleum ether, to separate the formed triphenylphosphine oxide as quantitatively as possible. To Purification of the petroleum ether Phase, the reaction product is obtained as a residue after evaporation of the petroleum ether. It can optionally be a high vacuum distillation be subjected.

The products of the process produced according to the invention are partially valuable substances with vitamin A activity, or they are also suitable as Food colors and feed additives.

Example 1 10.3 parts by weight triphenylphosphine-2-methyl-3-carbomethoxypropene- (2) -ylene- (1) are finely powdered and together with 0.05 parts by weight of phenothiazine in 20 parts by volume suspended in anhydrous acetonitrile. This is added with stirring in a nitrogen atmosphere a solution of 5.41 parts by weight of ß-dehydrojonylideneacetaldehyde at room temperature and 0.03 part by weight of phenothiazine in 10 parts by volume of anhydrous acetonitrile, the mixture is stirred at this temperature for a further 1 hour and then warms the batch to 85 ° C. After 3 hours, the reaction mixture is cooled and becomes a mixture poured from 50 parts by weight of ice and 20 parts by volume of 100 / above phosphoric acid. The reaction product is taken up in petroleum ether and the petroleum ether phase is washed neutral and dry them at 0 ° C over anhydrous sodium sulfate. After evaporation of the solvent, 7.5 parts by weight of vitamin A2 acid methyl ester are obtained as orange Oil that can be purified by high vacuum distillation. Kp.0001 = 155 to 1650 c (air bath temperature), yield 6.8 parts by weight (87 lo of theory).

C21 H28 Q2 (molecular weight 312.4): calculated. C 80.74 ° / o; H 9.040 / o; found . . C 80.54 ° / o, H 8.850 / 0. i = / lx = 377 ml (e = 35,000); Secondary maximum at 307 mm (e = l3000).

Example 2 To a suspension of 13.1 parts by weight of triphenylphosphine-2-methyl-3-carbomethoxypropene- (2) -ylene- (l) and 0.06 part by weight of phenothiazine in 23 parts by volume of tetramethylene sulfone and 3 Parts by volume of absolute benzene are left under nitrogen and with stirring at 200 C a solution of 6.9 parts by weight of F1-dehydrojonylidene acetaldehyde and 0.04 part by weight Phenothiazine in 11 parts by volume of tetramethylene sulfone and 2 parts by volume of absolute benzene flow in. The mixture is then stirred for a further hour at 200 ° C. and heated 800 C and maintains this temperature for 2 hours. The reaction mixture is then cooled and, as described in Example 1, worked up. 9 parts by weight of vitamin A2 acid methyl ester are obtained as an orange oil. This corresponds to a yield of 906% of theory. Of the Ester shows all of the chemical and physical properties of the previous example obtained substance.

Example 3 A suspension of 9.6 parts by weight of triphenylphosphine 2 -methyl- 3 - cyanopropene (2) -ylen- (1) and 10.05 parts by weight phenothiazine in 20 parts by volume anhydrous acetonitrile is stirred in a Nitrogen atmosphere at 200 C within 10 minutes with a solution of 5.4 Part by weight, B-dehydrojonylidene acetaldehyde and 0.03 part by weight phenothiazine added in 10 parts by volume of anhydrous acetonitrile. The mixture is then stirred another 1 hour at 200 C, then heats it to 800 C and maintains this temperature for 2.5 Hours. The cooled reaction mixture is worked up as described in Example 1 and dried at - 200 C over sodium sulfate. After evaporation of the Solvent 6.5 parts by weight of vitamin A2-acid nitrile, which is obtained by high vacuum distillation can be cleaned. 6.0 parts by weight (860% of theory) fall as red-orange tough oil on. Kp 0 OOt = 155 to 1650 C (air bath temperature). x "zlx = 373 mF (e = 32000); Secondary maximum at 304 m p (E = 13,000). The infrared absorption spectrum shows a sharp absorption at 2210 cm-1 for an α, ß-unsaturated nitrile group is characteristic.

C20H25N (molecular weight 279.4): calculated. C 85.97 ° / o, H 9.02 ° / o; found . . C 85.430 / o, H 9.07%.

Claims (1)

PATENT CLAIM: Process for the production of vitamin A2-acid nitrile or esters, characterized in that p-dehydrojonylidene acetaldehyde is combined with isolated, resonance-stabilized triphenylphosphine methylenes of the general formula wherein R denotes a cyano, carbalkoxy, carbocycloalkoxy or carbaryloxy radical, is reacted in a strongly polar solvent at elevated temperature, optionally in the presence of antioxidants and in the absence of oxygen.