理解异烟肼和耐药作用机制的计算方法

Lingaraja Jena, G. Wankhade, Pranita J Waghmare, B. Harinath
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引用次数: 5

摘要

大多数耐多药和极耐药结核分枝杆菌临床菌株对异烟肼和利福平等抗结核药物具有耐药性。异烟肼的作用机制和耐药性一直是人们广泛研究的课题。根据结核病耐药突变数据库,与异烟肼耐药相关的基因/蛋白有katG、nat、inhA、ahpc、ndh、kasA等22个。该基因的突变似乎影响异烟肼形成其活性形式或增强分解代谢,从而使其无效。不同实验室的研究表明,计算方法在阐明异烟肼的作用机制和耐药性的发展方面是有用的。我们实验室的计算研究表明,KatG (S315T/S315N)的突变可以阻止自由基的形成,从而产生对药物的耐药性。此外,我们通过分子动力学模拟方法观察到,NAT酶的突变(G67R/G207E)增加了突变酶的稳定性和催化能力,从而使药物失效。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Computational Approach in Understanding Mechanism of Action of Isoniazidand Drug Resistance
Most Multi Drug Resistance and Extremely Drug Resistance clinical strains of Mycobacterium tuberculosis are found to be resistant to the anti-tuberculousis drugs such as Isoniazid and Rifampicin. The mechanism of action and drug resistance due to Isoniazid has been the subject of extensive study. According to Tuberculosis drug resistance mutation database, 22 genes/proteins are associated with Isoniazid resistance such as katG, nat, inhA, ahpc, ndh, kasA etc. Mutation in the gene seems to affect the formation of Isoniazid to its active form or enhancing the catabolism thus making it ineffective. Studies in different laboratories have shown usefulness of computational approach in elucidating the mechanism of action of Isoniazid and development of drug resistance. Computational studies in our laboratory showed that a mutation in KatG (S315T/S315N) prevents free radical formation, thus the development of resistance to the drug. Further, we observed through molecular dynamics simulation approach that mutation (G67R/G207E) in NAT enzyme increases the stability and catalytic ability of the mutant enzyme, thus making the drug ineffective.
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