双孢蘑菇酪氨酸酶辅助合成L-多巴

Yu. A. Shesterenko
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引用次数: 0

摘要

左旋多巴(3,4-二羟基苯基-L-丙氨酸)是治疗帕金森病的首选药物。然而,它的化学合成方法有很多缺点,因此正在探索生物技术方法作为一种替代方法。目标目标是开发一种新的、负担得起的、有效的利用蘑菇酪氨酸酶生物合成L-DOPA的方法,该方法使用经济的载体固定化,以确保稳定性和酶的多种用途。方法。采用双孢蘑菇分离的酪氨酸酶进行研究。L-DOPA的生物合成是在水性和有机介质中进行的。使用质谱法、比旋转和熔点对所获得的产物进行分析。在聚N-乙烯基吡咯烷酮(PVP)中进行了酶的固定化,确定了与载体的相互作用、最适pH值和应用频率。后果从双孢蘑菇中分离得到一种部分纯化的酪氨酸酶制剂。在酶存在的水溶液中,由于随后形成复杂的多环化合物,仅获得5.1%的L-DOPA。在二氯甲烷中通过添加缓冲溶液生物合成L-DOPA衍生物,可以获得产率为55%的产物。固定化在PVP中的酪氨酸酶在CH2Cl2培养基中的活性比游离的高30%,并进行了7个循环的生物催化。结论。开发了一种使用基于固定化酪氨酸酶的可用生物催化剂合成L-DOPA的方法,该方法能够在二氯甲烷介质中使用7个循环获得L-DOPA。
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L-DOPA BIOSYNTHESIS WITH Agaricus bisporus TYROSINASES ASSISTANCE
L-DOPA (3,4-dihydroxyphenyl-L-alanine) is a drug of choice in Parkinson's disease treatment. However the chemical method of its synthesis has a number of drawbacks, so biotechnological approaches are being explored as an alternative. Aim. The goal is to develop a new affordable and effective method of biosynthesis of L-DOPA using mushroom tyrosinase, immobilized using an economical carrier, which ensures stability and enzyme multiple uses. Methods. Agaricus bisporus isolated tyrosinase was used in the work. L-DOPA biosynthesis was carried out in aqueous and organic medium. The obtained product was analyzed using mass spectrometry, specific rotation and melting point. The enzyme immobilization was carried out in poly-N-vinylpyrrolidone (PVP), the interaction with the carrier, pH-optimum and the application frequency were determined. Results. A partially purified preparation of tyrosinase was isolated from Agaricus bisporus. In aqueous solution in enzyme presence, only 5.1% of L-DOPA was obtained due to the subsequent formation of complex polycyclic compounds. The biosynthesis of L-DOPA derivative in methylene chloride with the addition of a buffer solution made it possible to obtain a product with a yield of 55%. Tyrosinase immobilized in PVP showed activity 30% higher than free in CH2Cl2 medium and carried out biocatalysis for 7 cycles. Conclusions. A method of L-DOPA synthesizing using an available biocatalyst based on immobilized tyrosinase was developed, which enabled to obtain L-DOPA during 7 cycles of use in a methylene chloride medium.
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