Iturin A对斜纹夜蛾蛋白酶抑制机制的同源性和分子动力学研究

Q3 Computer Science
N. K. Papathoti, Dusadee Kiddeejing, J. Daddam, Toan Le Thanh, N. Buensanteai
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引用次数: 0

摘要

斜纹夜蛾(Spodoptera litura),也被称为刀虫,属于夜蛾科,是许多作物系统的严重祸害,被认为是亚洲热带农业最重要的昆虫之一。世界上主要的环境威胁是植物害虫,已经商业化的农药是剧毒的,不可生物降解的,可能会有额外的残留物对生态系统有害。害虫抗性的增强往往要求使用先进的、对环境友好的、可生物降解的活性农药。在目前的工作中,通过在硅模型中使用微生物代谢物蛋白酶抑制剂(Iturin A)来确定蛋白酶对斜纹夜蛾消化系统的意义。在本研究中,我们建立了一个基于已知晶体结构的2D1I蛋白酶序列结构比对的模型。采用PROCHECK、WHAT IF、PROSA、Validate 3D、ERRAT等软件对模型进行可靠性评估。为了寻找新的蛋白酶对接抑制剂,本研究采用Iturin a进行研究,并提交了所产生蛋白酶模型的PMDB ID,以鉴定新的蛋白酶对接抑制剂,其注册号为PM0082285。酶抑制剂相互作用的详细研究发现了相似的核心残基;GLU215、LEU216、LYS217和GLU237已被证实在配体的结合效能中起作用。最新的蛋白酶模型的同源性建模和对接实验将为构建针对夜蛾的广谱新型杀虫剂的逻辑方法提供有用的见解知识。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Identification of Protease Inhibition Mechanism by Iturin A against Agriculture Cutworm (Spodoptera litura) by Homology Modeling and Molecular Dynamics
Spodoptera litura, otherwise known as cutworm, belongs to the Noctuidae tribe, which is a severe scourge for numerous crop systems and is considered one of Asian tropical agriculture's most important insects. The world's leading environmental threats are plant pests, and the already commercialized pesticides are extremely poisonous and non-biodegradable and maybe additional residues harmful to the ecosystem. The increased resistance in pests often demands the need for advanced, active pesticides that are environmentally friendly and biodegradable. In the current work, the significance of proteases for the Spodoptera litura digestive system has been determined by the use of microbial metabolite protease inhibitor (Iturin A) in silico models. In the present study, we developed a model based on sequence structural alignment of known crystal structure 2D1I protease from Homo sapiens. The model's reliability evaluation was performed using programs such as PROCHECK, WHAT IF, PROSA, Validate 3D, ERRAT, etc. In an attempt to find new inhibitors for Protease docking, the study was carried out with Iturin A. PMDB ID for the produced protease model was submitted to identify new inhibitors for Protease docking, and its accession number is PM0082285. The detailed study of enzyme-inhibitor interactions identified similar core residues; GLU215, LEU216, LYS217, and GLU237 have demonstrated their role in the binding efficacy of ligands. The latest homology modeling and docking experiments on the protease model will provide useful insight knowledge for the logical approach of constructing a wide spectrum of novel insecticide against Spodoptera.
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来源期刊
Open Bioinformatics Journal
Open Bioinformatics Journal Computer Science-Computer Science (miscellaneous)
CiteScore
2.40
自引率
0.00%
发文量
4
期刊介绍: The Open Bioinformatics Journal is an Open Access online journal, which publishes research articles, reviews/mini-reviews, letters, clinical trial studies and guest edited single topic issues in all areas of bioinformatics and computational biology. The coverage includes biomedicine, focusing on large data acquisition, analysis and curation, computational and statistical methods for the modeling and analysis of biological data, and descriptions of new algorithms and databases. The Open Bioinformatics Journal, a peer reviewed journal, is an important and reliable source of current information on the developments in the field. The emphasis will be on publishing quality articles rapidly and freely available worldwide.
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