BE492555A - - Google Patents

Description

       

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  "New substance generating vitamin D3".



   The Applicant Company has announced, in a previous patent, the separation of a new substance which generates vitamin D2 or calciferol. New research has enabled it to achieve a similar result in the field of vitamin D3 The subject of the present invention is therefore a new substance to which the applicant gives the name of previtamin D3 and the use of which is intended as generator body for industrial preparation

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 vitamin D3
A first process for obtaining this substance consists in preparing in the usual way the irradiation resin from 7 - de-hydrocholesterol, then with the ester, for example with dinitro-3, 5-benzoyl chloride. ,

   taking care not to exceed the temperature of 25 at all stages of the preparation. Chromatoraphic separation is then carried out on neutral alumina. From the less strongly adsorbed fraction, an amber oil is separated which
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 little by little crystallizes under ligrolne. The previtamin un D3 is thus isolated in the form of a dinitrobenzoate with a yield of the order of 50% relative to the resin used.



   As shown by centesimal analysis and cryoscopy,
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 this previtamin D3 dinitrobenzoate, C34H4606NZ is an isomer of vitamin D3 dinitrobenzoate Analysis:
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 Calculated elo 70.55 Hbo 8eO N% z M. 579 Found 70.5 7.85 4.9 555
The new substance is unequivocally distinguished from vitamin D3 dinitro-benzoate, just as it cannot be confused with any of the derivatives already described in the genesis of this vitamin.



  The table below gives the physical constants published in the literature and those determined by the applicant, allowing those to be compared with / of previtamin D3 dinitrobenzoate.
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  : 7-dehydrocholesterol: Lumisterol 3: Tachysterol 3
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<tb>: <SEP> (dinitrobenzoate) <SEP> (dinitrobenz .: <SEP> (noun <SEP> amorph. <SEP>)
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<tb> F.
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  (inst.) <SEP>; <SEP> 207 <SEP> 131
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 (oc) D -46 (CHCL3): +20 (CHCL3): -11 (CHCL3): Previtamin D3 Vitamin D3
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<tb> (dinitrobenz. <SEP>) <SEP>. <SEP> (dinitrobenz.). <SEP>
<tb>
 
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  F, 110-111: 1420 and 150: 7 (inst). (dimorphic) (o () D +52 (CHCL3) +97 (CHCL3): +380 (C 6 H6)> 62e (06H6):

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Previtamin D3 dinitrobenzoate crystallizes in very pale yellow fine needles. So far the best solvent which has made it possible to separate it has been methyl ethyl ketone.



   The 10-15 alkaline saponification of the dinitrobenzoate results in previtamin D3 in an amorphous state. The specific optical rotation of this substance for the D line is close to +40 (c = 1% in benzene), while it is +83 for vitamin D3
When subjected to the action of chlorides or acid anhydrides, previtamin D3 provides esters, the most interesting of which appears to be the dinitrobenzoate already mentioned. Pre-vitamin D3 does not precipitate digitonin.



   This new substance, obtained by saponification of its dinitrobenzoate, offers an evolution of its optical rotation under the influence of heating in solvent. It gives rise to vitamin D3 without requiring the supply of light energy.



   As for the precalciferol forming the subject of the preceding invention, the Applicant has observed that previtamin D3 could also be obtained by a second process based on the following observation: the transformation of previtamin into vitamin of offers a character of reversibility.



   Consequently, if moderately heated, for example at 60 for 20 hours, a benzene solution of vitamin D dinitrobenzoate, the optical rotation, for the D line, changes in the direction of a slight decrease from +62 to +58. Fractional crystallizations and chromatography provide previtamin D dinitrobenzoate which, by saponification, in turn leads to previtamin d3 However, in this case, the balance of the two substances still being strongly shifted in favor of the vitamin, the yield in previtamin is obviously much lower than that of the direct process.

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   Various modes of preparation of previtamin D3 are given below, by way of examples, but without limitation. EXAMPLE 1
Direct process (Preparation of previtamin D3 from the irradiation resin of 7-dehydrocholesterol).



   50 g of 7-dehydrocholesterol dissolved in 5,000 cm3 of sulfuric ether are irradiated for one hour under a nitrogen atmosphere at a temperature of 16 by the light of the magnesium spark After distillation of the ether under vacuum below 10-15, the unconverted 7-dehydrocholesterol (32 g) is removed by taking up in methanol in which it is very slightly soluble. After evaporation of the methanol under vacuum at 50, the residual oil is freed of the last traces of methanol by several times with benzene. The resin obtained (17 g) is esterified over 1 hour at 15 in benzene solution with dinitro-3,5-benzoyl chloride in the presence of pyridine.

   After washing the benzene solution with 10% sodium bicarbonate solution, with water and then with dilute hydrochloric acid, the benzene is removed under reduced pressure to 10-15. The oily crude dinitrobenzoate is taken up several times in petroleum ether to remove the last traces of benzene and then finally dissolved in 1200 cm 3 of petroleum ether. After standing overnight in a cooler, a slight insoluble material is separated by filtration and then chromatography on a column of 375 g of neutral alumina. The chromatogram was developed by washing with petroleum ether until the yellow color reached the bottom of the column.



  Washing is continued with petroleum ether and the filtrate is collected until the second yellow ring, a little darker, reaches the bottom of the column. The filtrate is concentrated to small volume by distillation under reduced pressure to 10-15. 7.1 g of previtamin D3 dinitrobenzoate separated in fine white-yellowish needles F. 110-111 (block), (o () D = + 38 (benzene, c = 1%).

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 the stock solution and add 3 times a volume of absolute alcohol.



  It separates a second less pure jet, 2.25 g. F. 106-107 (block).



  The yield therefore exceeds 50% by weight relative to the resin free from 7-dehydrocholesterol and not esterified.



   The free previtamin is obtained from its dinitrobenzoate by alkaline saponification, according to the usual methods, but taking care to always maintain the temperature below 15, EXAMPLE 2
Indirect process (obtaining previtamin D3 from vitamin D3 dinitrobenzoate)
2.9 g of vitamin D3 dinitrobenzoate are dissolved in 30 cm3 of benzene and heated for 15 hours at 60 in the dark.



  The henzene is removed completely under reduced pressure at a temperature below 20. Peprend with 30 cm3 of petroleum ether at 20 and the insoluble matter is filtered off. 1.55 g of vitamin D3 F.149 dinitronenzoate (block) are thus collected. The stock solution concentrated to 20 cm3 provides a second stream of 0.35 g of vitamin D3'F dinitrobenzoate 149 (block) *
The stock solution is then chromatographed on 20 g of neutral alumina. Pqr washing with petroleum ether as in Example 1, 0.3 g of previaamine D3 dinitrobenzoate, F. 110 (block) is collected.



  Washing the alumina with ether elutes 0.5 g of vitamin D3 dinitrebenzoate.



   In total, the following were separated: 0.3 g of previtamin D3 'F 110 dinitrobenzoate (block), (Ó) D20 = +38.5 (benzene, c 1%), or 10% by weight of vitamin D3 dinitrobenzoate , starting and recovered 2.4 g of vitamin D3 dinitrobenzoate, F. 1490 (block), (Ó) D = +62 (benzene, c = 1%), or 83% of the amount involved.



  EXAMPLE 3 (Preparation of vitamin D3 from previtamin D3 without input of light energy and under the sole influence of moderate heating)

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A 1% benzene solution of previtamin D3 dinitrobenzoate is heated at 60, for example, for twenty hours and protected from light, It is also possible to proceed on this solution, to very types of heating, at 40 for example for two days, or at 80 for two to three hours. The higher the temperature, the shorter the duration of the transformation that is sought: in practice it seems preferable not to exceed 80 to avoid too significant resinification.



   At the start of the experiment, the specific optical rotation is that of previtamin D3 dinitrobenzoate to benzene, i.e. +38.5.



  Gradually, this power evolves in the direction of an increase and at the end of the test it reaches a value quite close to that of pure vitamin D3 dinitrobenzoate, in general +58. It suffices to distill the benzene under reduced pressure, then to recrystallize in the usual manner to separate the pure vitamin D3 dinitrobenzoate, m.p. 149-150; (block), (Ó) D - +62 (benzene) with a yield of 70 to 80%. Vitamin D3 is finally obtained by saponifying its dinitrobenzoate in the usual manner.



   In the above experiment, the starting material was previtamin D3 dinitrobenzoate. The preparation can also be carried out also by simple heating starting from the free previtamin, obtained by saponification of its dinitrobenzoate. The optical rotation of previtamin D3 in benzene solution is lower than that of vitamin D3, +40 instead of + 83.

   By carrying out the heating test as has just been indicated, the increase in optical rotation leads, at the end of the test, to a value of the order of +70. The usual concentrations and recrystallizations then make it possible to separate vitamin D3 It is also possible to proceed to the direct esterification of the heated product with dinitrobenzoyl chloride and to collect in excellent yield the pure vitamin D43 dinitrobenzoate from which the vitamin is liberated by saponification.

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   In both cases, the novel vitamin D3 generator which is the subject of the present invention therefore indeed supplied vitamin D3 under the influence of moderate heating, and in the absence of
3 light. Numerous variants can be adopted without the very principle of the preparation of vitamin D3 from the new generator, previtamin D3, being called into question.


    

Claims (1)

ABSTRACT The objects of the invention are: 1) As a new industrial product, a gene substance ratifying vitamin D3, isomer of the latter, called pre-vitamin D3, and exhibiting the characteristics and properties defined above; 2) as new industrial products, esters of the substance defined under 1), and in particular dinitrobenzoate; 3) a process for preparing the following substances 1 and 2 from 7-dehydrocholesterol which consists in preparing in the usual way, using the Mg spark, the irradiation resin of the esterifcer the 7-dehydrocholesterol resin , to separate the excess of 7-dehydrocholes6terol, for example by means of dinitro-3, 5-benzoyl, taking care not to exceed the temperature of 25 at all stages of the preparation, to separate by chromatography a fraction less strongly adsorbed to crystallize this less strongly adsorbed fraction using a solvent or mixture of solvents such as ligrolne, to separate the ester of previtamin D by further crystallization using a mixture of solvents or a solvent such as methyl ethyl ketone and alcohol then, finally, to be saponified with the alkalis according to the usual methods and at a temperature preferably not exceeding 15; 4) an indirect process for obtaining the following substances 1 and 2 which consists in subjecting to moderate heating, at a temperature preferably not exceeding 60, in the presence of a solvent such as benzene, an ester of vitamin D3, such as in particular the dinitrobenzoate of vitamin D3, then in separating the ester of previtamin D according to one or all of the phases of se- <Desc / Clms Page number 8> paration described under 3), finally in saponifying the ester as defined under 3); 5) a process for preparing vitamin D from the following substances 1 and 2 which consists of subjecting to moderate heating at a temperature preferably not exceeding 80, in the presence of a solvent such as benzene, previtamin d3 or one of its esters such as dinitrobenzoate, then separating the vitamin D3 or its ester in the usual manner.