解毒酶研究的分子对接

Rafael Trindade Maia and Vinícius Costa Amador
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引用次数: 2

摘要

在本章中,我们指出了在解毒超家族酶谷胱甘肽s -转移酶(GSTs)对杀虫剂和除草剂抗性的背景下,通过蛋白质-配体对接模拟获得的一些相关结果。我们在此提出了一些GST与疟疾和登革热媒介(冈比亚按蚊和埃及伊蚊)中的化学杀虫剂以及水稻(Oryza sativa)培养中使用的化学除草剂结合的硅证据。我们的研究结果表明,epsilon类的一些成员(GSTE2, GSTE5)可以代谢一些杀虫剂化合物,tau类成员(GSTU4)可以代谢一些除草剂。这一结果加强了对接研究对酶活性理解的重要性。这些信息可以使今后通过针对特定商品及服务税目标的生物技术改进,实施蚊虫控制和水稻栽培除草剂管理的新战略。gst4催化结合位点诱导突变可提高水稻抗除草剂能力,减少作物损失,设计合理的化合物抑制GSTE成员,降低蚊虫对杀虫剂的抗性。在这两种情况下,可以开发生物技术工具,重点放在商品服务税上,以减少使用杀虫剂和除草剂对环境的影响。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Molecular Docking for Detoxifying Enzyme Studies
In this chapter, we pointed some relevant results obtained by protein-ligand docking simulations in the context of insecticide and herbicide resistance performed by glutathione S-transferases (GSTs), a detoxifying superfamily enzyme. We present here some in silico evidences of GST binding against chemical insecticides in the malaria and dengue vectors ( Anopheles gambiae and Aedes aegypti mosquitoes) and against chemical herbicides used on rice ( Oryza sativa ) culture. Our findings suggest that some members from epsilon class (GSTE2, GSTE5) can metabolize some insecticide compounds and that a tau class member (GSTU4) can metabolize some herbicides. The results reinforce the importance of docking studies for enzyme activity comprehension. These information can allow in the future the implementation of new strategies for mosquito control and herbicide man-agement on rice culture through biotechnological improvements designed to specific GST targets. Induced mutations on catalytic binding sites of GSTU4 could improve rice herbicide resistance and minimize produce damage, while rational compounds can be designed to inhibit GSTE members to decline insecticide resistance on mosquito control. In both cases, biotechnological tools could be developed focusing on GSTs that would reduce environmental impact by the use of insecticide and herbicide.
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