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寡聚物形成与 Vip3Aa 毒素的杀虫活性。

Oligomer Formation and Insecticidal Activity of Vip3Aa Toxin.

机构信息

China National Engineering Research Center of JUNCAO Technology, College of Life Science, Fujian Agriculture and Forestry University, Fuzhou 350002, Fujian, China.

Key Laboratory of Biopesticide and Chemical Biology (Ministry of Education), College of Plant Protection, Fujian Agriculture and Forestry University, Fuzhou 350002, Fujian, China.

出版信息

Toxins (Basel). 2020 Apr 23;12(4):274. doi: 10.3390/toxins12040274.

Abstract

(Bt) Vip3A proteins are important insecticidal proteins used for control of lepidopteran insects. However, the mode of action of Vip3A toxin is still unclear. In this study, the amino acid residue S164 in Vip3Aa was identified to be critical for the toxicity in . Results from substitution mutations of the S164 indicate that the insecticidal activity of Vip3Aa correlated with the formation of a >240 kDa complex of the toxin upon proteolytic activation. The >240 kDa complex was found to be composed of the 19 kDa and the 65 kDa fragments of Vip3Aa. Substitution of the S164 in Vip3Aa protein with Ala or Pro resulted in loss of the >240 kDa complex and loss of toxicity in . In contrast, substitution of S164 with Thr did not affect the >240 kDa complex formation, and the toxicity of the mutant was only reduced by 35%. Therefore, the results from this study indicated that formation of the >240 kDa complex correlates with the toxicity of Vip3Aa in insects and the residue S164 is important for the formation of the complex.

摘要

(Bt) Vip3A 蛋白是一种重要的杀虫蛋白,用于防治鳞翅目昆虫。然而,Vip3A 毒素的作用模式仍不清楚。本研究鉴定出 Vip3Aa 中的氨基酸残基 S164 对于毒素的毒性至关重要。S164 取代突变的结果表明,Vip3Aa 的杀虫活性与蛋白酶激活后形成 >240 kDa 的毒素复合物相关。发现 >240 kDa 的复合物由 Vip3Aa 的 19 kDa 和 65 kDa 片段组成。用 Ala 或 Pro 取代 Vip3Aa 蛋白中的 S164 会导致 >240 kDa 复合物的丢失和在昆虫中的毒性丧失。相比之下,用 Thr 取代 S164 不会影响 >240 kDa 复合物的形成,突变体的毒性仅降低 35%。因此,本研究结果表明,>240 kDa 复合物的形成与 Vip3Aa 在昆虫中的毒性相关,而残基 S164 对于复合物的形成很重要。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/5543/7232161/def9c37f13cf/toxins-12-00274-g001.jpg

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