DE2063027A1 - Salt of a basic amino acid of 5 6,7,8 tetrahydrofolic acid - Google Patents

Description

Basic Amino Acid Salt of 5, 6, 7, 8-Tetrahydrofolic Acid The present invention relates to salts of basic amino acids of 5, 6, 7, 8-tetrahydrofolic acid (hereinafter the acid is abbreviated as "THFA") e THFA is represented by the formula and is an amphoteric material in terms of chemical structure and referred to as an active type of folic acid in vivo, THFA is an important material which contributes to in vivo functions such as homopoietic activity and liver protective activity.

THFA can be dissolved in water, but its aqueous solution is very unstable and THFA has not yet been isolated in pure crystals had to do this experimentally to produce an injection solution from THFA in order to cease the properties of a solution containing TIIFA, e.g. the TlIFA as a reaction product with an alkali or the like. However, from a purity standpoint, this is undesirable as a medicament and represents a considerable deficiency for commercial exploitation, as the salt of the THFA only the sulfate has been isolated in pure crystals. An aqueous solution of the However, salt is unsuitable as a solution for injection because of the acidity of the aqueous Solution is too strong.

Based on these technological facts, it is very desirable Isolate THFA in such a form from which a solution for injection is easily made can be, this means from a form that is stable and easily soluble in water is, An object of this invention is to provide a salt of the basic amino acid of the THFA available, which is stable, easily soluble in water and very can be easily processed into a solution for injection, As a result of various Investigations have been found that the salt of a basic amino acid of the THFA, made by reacting THFA and 2 moles of a basic amino acid, is unexpectedly stable and easily soluble in water, the salt is quite economical can be used for the production of preparations, especially for injection solutions and meets the above requirement, for the production of the salt of a basic Amino acid of the THFA of this invention becomes crude THFA by catalytic reduction of folic acid (see Biochem. Prep. 7, 89-92 (1960)), in a reaction solvent suspendedb An aqueous solution containing more than 2 equivalents of a basic amino acid is added to the suspension, preferably in a nitrogen gas stream, The isolation of the desired material from the reaction solution is carried out by adding an organic solvent in which the desired Material is sparingly soluble or insoluble and where the organic solvent is sufficiently miscible with water, such as ethanol, acetone, dioxane and the like. Through this the desired material will be deposited and the precipitates thus formed will be obtained in a known manner such as filtration or by centrifugal separation, The desired material thus obtained has sufficient purity and can be used as Raw material to be used in the manufacture of preparations. Additionally was ensured by investigations by means of paper chromatography that the desired Material is present as the only compound, As a basic amino acid, dia in this one Invention can be used, may be mentioned for clarification L-arginine, L-ornithine and L-lysine, as the reaction solvent can be water, water-containing alcohols and the like can be used. It is preferred to previously add air dissolved therein or remove a reducing agent, such as a sulfite, to the reaction solvent added before it is used for the reaction.

Examples are given below to illustrate the invention.

Example 1 In 20 ml of deoxygenated water, 4.81 g crude 5,6,7,8-tetrahydrofolic acid produced by a known method was suspended. While stirring the suspension and while passing in nitrogen became a solution of 3.48 g of L-arginine in 20 ml of deoxygenated water slowly added to the suspension, the reaction product solution being a light yellow results in a transparent solution. When the solution was further stirred for about 20 minutes and then add 100 ml of ethanol was added to the reaction product solution, an oily material was obtained. 5, 6, 7, 8-tetrahydrofolic acid. L-arginine was precipitated as a light yellow powder when adding 50 ml of ethanol to the oily material was added. The powder was purified by filtration under pressure in a nitrogen atmosphere separated, it was 8.2 g of the product with a melting point of 195-197 ° C under Decomposition obtained after drying.

Elemental analysis as C31 H51 N15 O10 'H2O: Calculated: C 44.87%, H. 6.6, N 25.32% Found: C45.08%, H6.47%, N 25.12% The product has ultraviolet absorption at a max at 297 mu and a min at 243 mu, which is with the ultraviolet absorption which corresponds to 5, 6, 7, 8-tetrahydrofolic acid.

Example 2 purch Repeat the same procedure as in the example 1, but using 2.92 g of L-lysine instead of L-arginine became 5, 6, 7, 8-tetrahydrofolic acid. L-lysine obtained in almost quantitative yield.

Melting point: 189 - 191 ° C (with decomposition) Elemental analysis as C31 H51 N11 O10 'H2O: Calculated: C 48.12%, H 7.16%, N 19g9lfo Found: $ C48.36%, H 6.95%, N 20.21% Example 3 4S96 was added to 20 ml of deoxygenated water g 5, -Methyl-5, 6, 7, 8-tetrahydrofolic acid. Suspended dihydrate with stirring nitrogen was passed into the suspension 0 A solution of 3.4 g of L-arginine in 20 ml of Oxygen freed water to the Suspension added, a slightly yellow transparent solution was obtained. if the reaction product solution was further stirred for 20 minutes and then 100 ml of ethanol was added to the reaction product solution, an oily material was obtained When 50 ml of ethanol was added to the oily material, 5-methyl-5, 6, 7, 9-tetrahydrofolic acid, l-arginine deposited as a light yellow powder. The powder was separated by filtration under pressure in a nitrogen stream and dried It was 8.3 g of product with a melting point of 127 - 1300 G (with decomposition) obtain.

Elemental analysis as C32 H53 H15 O10 '2 H2O: Calculated: C45.55%, H6.8%, N24.90% Found: C45.93%, H6.67%, N 25.18% The product has an ultraviolet absorption at a max at 290 mu and a min at 245 mu, which is with the ultraviolet absorption of 5-methyl-5, 6, 7, 8-tetrahydrofolic acid, Example 4 When 4.96 g 5-methyl-5, 6, 7, 8-tetrahydrofolic acid dihydrate was reacted with 2.64 g of L-ornithine and was described in the same way as in Example 3, 5-methyl-5, 6, 7, 8-tetrahydrofolic acid. L-ornithine obtained almost quantitatively.

Melting point: 149-155 "C (with decomposition), elemental analysis as C30 H49 H11 O10 '2 H2O: Calculated: C47.42%, H7.03%, N20.28% Found: C47.72%, H. 7.03%, N20.50%

Claims (1)

Claims: @@). 0 Salt of a basic amino acid of 5, 6, 7, 8-tetrahydrofolic acid with the formula 2.) Salt of a basic amino acid according to claim 1, which contains L-arginine as the basic amino acid. 3,) Salt of a basic amino acid according to claim 1, werin as basic Amino acid L-lysine is contained, 4.) Salt of a basic amino acid according to claim 1, which contains L-ornithine as the basic amino acid. 5,) Use of a salt of a basic amino acid liter of 5,6,7,8-tetrahydrofolic acid according to one of claims 1 to 4 as an active ingredient for the preparation of aqueous injection solutions for the treatment of humans and animals. 6.) Use of a salt of a basic amino acid of 5, 6, 7, 8-Tetrahydrofolic acid according to one of Claims 1 to IF as an active ingredient for production of pharmaceutical preparations with homopoetic and liver protective activity for the treatment of humans and animals.