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基于结构的虚拟筛选鉴定及 Vip3Aa 关键残基在鳞翅目昆虫刷状缘受体结合中的验证

In Silico Structure-Based Identification and Validation of Key Residues of Vip3Aa Involving in Lepidopteran Brush Border Receptor Binding.

机构信息

Northeast Agricultural University, Harbin, 150030, People's Republic of China.

出版信息

Appl Biochem Biotechnol. 2019 Apr;187(4):1448-1459. doi: 10.1007/s12010-018-2880-6. Epub 2018 Sep 25.

Abstract

The vegetative insecticidal proteins (VIPs) of Bacillus thuringiensis (Bt) have a broad-spectrum insecticidal activity against Lepidopteran pests and no cross-resistance with the insecticidal crystal protein Cry protein. So there are great potentials for the control of agricultural pests and the resolution of resistance problems. The structural information of Vip3Aa protein and the predicted key amino acid sites on the C-terminal domain of Vip3Aa were analyzed with the methods of bioinformatics such as homology modeling and molecular docking. Site-directed mutagenesis was used to replace these amino acids with alanine, and there was difference in the activities of the mutant protein and Vip3Aa protein. Y619A had improved insecticidal activity against Helicoverpa armigera, but the toxicity of W552A and E627A to Helicoverpa armigera was significantly reduced. The mutants of W552A and E627A had reduced insecticidal activity against Spodoptera exigua. This study demonstrated that the C-terminal domain played an important role in the function of Vip3Aa protein toxin, and the deletion of the side chain of key residues had a significant effect on the activity of the insecticidal protein. This study provides the theoretical basis for revealing the relationship between the structure and function of Vip3Aa protein.

摘要

苏云金芽孢杆菌(Bt)的杀虫晶体蛋白(Cry)对鳞翅目害虫具有广谱杀虫活性,与杀虫晶体蛋白 Cry 蛋白无交叉抗性。因此,在农业害虫防治和解决抗性问题方面具有巨大的潜力。本研究采用同源建模和分子对接等生物信息学方法分析了 Vip3Aa 蛋白的结构信息和 Vip3Aa 蛋白 C 末端结构域上预测的关键氨基酸位点。通过定点突变将这些氨基酸突变为丙氨酸,突变蛋白与 Vip3Aa 蛋白的活性存在差异。Y619A 对棉铃虫的杀虫活性提高,但 W552A 和 E627A 对棉铃虫的毒性显著降低。W552A 和 E627A 的突变体对斜纹夜蛾的杀虫活性降低。本研究表明 C 末端结构域在 Vip3Aa 蛋白毒素功能中起重要作用,关键残基侧链的缺失对杀虫蛋白的活性有显著影响。本研究为揭示 Vip3Aa 蛋白的结构与功能关系提供了理论依据。

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