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球形芽孢杆菌晶体杀幼虫毒素中毒性决定因素的鉴定及分子结构预测分析

Identification and molecular structural prediction analysis of a toxicity determinant in the Bacillus sphaericus crystal larvicidal toxin.

作者信息

Yuan Z, Rang C, Maroun R C, Juárez-Pérez V, Frutos R, Pasteur N, Vendrely C, Charles J F, Nielsen-Leroux C

机构信息

CIRAD, Montpellier, France.

出版信息

Eur J Biochem. 2001 May;268(9):2751-60. doi: 10.1046/j.1432-1327.2001.02176.x.

DOI:10.1046/j.1432-1327.2001.02176.x
PMID:11322897
Abstract

The operon containing the genes encoding the subunits of the binary crystal toxin of Bacillus sphaericus strain LP1-G, BinA and BinB (41.9 kDa and 51.4 kDa, respectively), was cloned and sequenced. Purified crystals were not toxic to Culex pipiens larvae. Comparison of the amino-acid sequences of this strain (Bin4) with those of the three other known toxin types (Bin1, Bin2 and Bin3) revealed mutations at six positions, including a serine at position 93 of BinA4, whereas all other types of BinA toxin from B. sphaericus had a leucine at this position. Reciprocal site-directed mutagenesis was performed to replace this serine in BinA4 from LP1-G with a leucine and the leucine in the BinA2 protein from strain 1593 with a serine. Native and mutated genes were cloned and overexpressed. Inclusion bodies were tested on C. pipiens larvae. Unlike the native Bin4 toxin, the mutated protein was toxic, and the reciprocal mutation in Bin2 led to a significant loss of toxicity. In vitro receptor-binding studies showed similar binding behaviour for native and mutated toxins. In the absence of any experimental data on the 3D structure of these proteins, sequence analysis and secondary-structure predictions were performed. Amino acid 93 of the BinA polypeptide probably belongs to an alpha helix that is sensitive to amino-acid modifications. Position 93 may be a key element in the formation of the BinA-BinB complex responsible for the toxicity and stability of B. sphaericus Bin toxins.

摘要

对包含球形芽孢杆菌菌株LP1-G二元晶体毒素亚基(BinA和BinB,分子量分别为41.9 kDa和51.4 kDa)编码基因的操纵子进行了克隆和测序。纯化的晶体对致倦库蚊幼虫无毒。将该菌株(Bin4)的氨基酸序列与其他三种已知毒素类型(Bin1、Bin2和Bin3)的序列进行比较,发现六个位置存在突变,包括BinA4第93位的丝氨酸,而球形芽孢杆菌的所有其他类型的BinA毒素在该位置为亮氨酸。进行了相互的定点诱变,将LP1-G的BinA4中的该丝氨酸替换为亮氨酸,将1593菌株的BinA2蛋白中的亮氨酸替换为丝氨酸。对天然基因和突变基因进行了克隆和过表达。对包涵体在致倦库蚊幼虫上进行了测试。与天然的Bin4毒素不同,突变蛋白具有毒性,而Bin2中的相互突变导致毒性显著丧失。体外受体结合研究表明,天然毒素和突变毒素具有相似的结合行为。在没有这些蛋白质三维结构的任何实验数据的情况下,进行了序列分析和二级结构预测。BinA多肽的第93位氨基酸可能属于对氨基酸修饰敏感的α螺旋。93位可能是负责球形芽孢杆菌Bin毒素毒性和稳定性的BinA-BinB复合物形成中的关键元件。

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