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对映选择性脂肪酶的定向进化

Directed evolution of an enantioselective lipase.

作者信息

Liebeton K, Zonta A, Schimossek K, Nardini M, Lang D, Dijkstra B W, Reetz M T, Jaeger K E

机构信息

Lehrstuhl für Biologie der Mikroorganismen, Ruhr-Universität, Bochum, Germany.

出版信息

Chem Biol. 2000 Sep;7(9):709-18. doi: 10.1016/s1074-5521(00)00015-6.

Abstract

BACKGROUND

The biocatalytic production of enantiopure compounds is of steadily increasing importance to the chemical and biotechnological industry. In most cases, however, it is impossible to identify an enzyme that possesses the desired enantioselectivity. Therefore, there is a strong need to create by molecular biological methods novel enzymes which display high enantioselectivity.

RESULTS

A bacterial lipase from Pseudomonas aeruginosa (PAL) was evolved to catalyze with high enantioselectivity the hydrolysis of the chiral model substrate 2-methyldecanoic acid p-nitrophenyl ester. Successive rounds of random mutagenesis by ep-PCR and saturation mutagenesis resulted in an increase in enantioselectivity from E=1.1 for the wild-type enzyme to E=25.8 for the best variant which carried five amino acid substitutions. The recently solved three-dimensional structure of PAL allowed us to analyze the structural consequences of these substitutions.

CONCLUSIONS

A highly enantioselective lipase was created by increasing the flexibility of distinct loops of the enzyme. Our results demonstrate that enantioselective enzymes can be created by directed evolution, thereby opening up a large area of novel applications in biotechnology.

摘要

背景

对化学和生物技术产业而言,对映体纯化合物的生物催化生产正变得越来越重要。然而,在大多数情况下,无法鉴定出具有所需对映选择性的酶。因此,迫切需要通过分子生物学方法创建具有高对映选择性的新型酶。

结果

对铜绿假单胞菌的一种细菌脂肪酶(PAL)进行改造,使其能够以高对映选择性催化手性模型底物对硝基苯基2-甲基癸酸酯的水解反应。通过易错PCR进行连续轮次的随机诱变和饱和诱变,使得对映选择性从野生型酶的E=1.1提高到携带五个氨基酸取代的最佳变体的E=25.8。最近解析的PAL三维结构使我们能够分析这些取代的结构后果。

结论

通过增加酶特定环的柔韧性创建了一种高对映选择性脂肪酶。我们的结果表明,可以通过定向进化创建对映选择性酶,从而在生物技术领域开辟大量新的应用。

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