Highly concentrated preparations of dopa compounds

Drug – bio-affecting and body treating compositions – Antigen – epitope – or other immunospecific immunoeffector – Parasitic organism or component thereof or substance...

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424274, 424319, A01N 3713

Patent

active

044092334

DESCRIPTION:

BRIEF SUMMARY
TECHNICAL FIELD

This invention relates to a process for preparing a highly concentrated preparation of dopas known as a remedy for Parkinson's disease or a hypotensive agent.


BACKGROUND ART

Typical examples of a dopa include dopa [.beta.-(3,4-dihydroxyphenyl)-.alpha.-alanine] and methyldopa [L-3-(3,4-dihydroxyphenyl)-2-methylalanine]. The former is known as a remedy for Parkinson's disease and the latter is known as a hypotensive agent. These compounds, however, have poor solubility in water and are inconvenient to be used in the form of a solution, particularly an injection. For example, the solubility of dopa in water is 2.5 mg/ml and 20 ml of water is necessary to dissolve the minimal dose (50 mg of dopa). Such circumstances require large ampules which are inconvenient for use. Therefore, preparations containing these compounds at a high concentration have been desired. Heretofore, there have been known attempts for the preparation of a highly concentrated dopa preparation; U.S. Pat. Nos. 3,916,004 and 3,911,137. The former comprises reacting a dopa with a non-toxic polyvalent metal salt to form a complex and the latter comprises adding a high molecular weight compound to a dopa to dissolve the dopa at a high concentration. However, the concentration of the dissolved dopa in these two inventions has not yet been sufficient to meet the requirement in the pharmaceutical field and there has been a demand for a process for preparing a much more highly concentrated dopa preparation. This invention provides a process for preparing a far more highly concentrated dopa preparation than made in a prior art. Also, another object of this invention is to provide a highly concentrated preparation of a dopa compound in the form of an aqueous solution or a freeze-dried preparation thereof.


DISCLOSURE OF INVENTION

As a result of further studies to dissolve a dopa compound in water at a high concentration, the present inventors have found that a dopa can be dissolved in a high concentration (10-100 mg/ml) by adding a basic amino acid and/or a certain type of a neutral amino acid to the dopa compound and also that a freeze-dried preparation of the highly concentrated solution thus prepared can be readily redissolved in distilled water for injection when used to reproduce the original high concentration of a dopa compound and can be kept stable at room temperature or even in a cold place. The present invention has been completed upon the above-mentioned findings. Thus, the present highly concentrated preparation of a dopa may be formulated and used in the form of an aqueous solution or a freeze-dried preparation therefrom. The basic amino acid which may be employed in this invention is not critical and may be any type and sort of the basic amino acids now available. Preferable examples thereof may include arginine, lysine, histidine and ornithine.
The neutral amino acid which may be employed in this invention is methionine, proline, hydroxyproline, serine, threonine or valine. In view of solubility, stability and the like, arginine, lysine, ornithine, methionine, serine, proline, hydroxyproline, threonine and valine are preferable. Also, these amino acids may be used alone or in combination of two or more thereof. A concentration of the amino acid to be added is dependent upon solubility of the additive, but 1-300 mg/ml is effective. Excessively high concentrations of the amono acid may cause coloration. In order to stabilize the active ingredient (a dopa), it is preferred to incorporate ascorbic acid or sulfites into the preparation of this invention. Furthermore, in the case of an injectable preparation, such additives as an isotonic agent, an antiseptic agent or a preservative commonly employed in an injectable preparation may be optionally added to the preparation of this invention, examples of such additives being sodium chloride, methylparaben, propylparaben, benzethonium chloride, benzalkonium chloride and the like.
Moreover, a far more highly concentrated preparation of a dopa (at 50 mg/ml) can be produced b

REFERENCES:
patent: 3911137 (1975-10-01), Miki et al.
patent: 4321264 (1982-03-01), Vickers

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