Characterization of the individual domains of the Bacillus thuringiensis Cry2Aa implicates Domain I as a possible binding site to Helicoverpa armigera

IF 3.6 3区 生物学 Q1 ZOOLOGY Journal of invertebrate pathology Pub Date : 2024-05-14 DOI:10.1016/j.jip.2024.108129
Meng Meng , Cheng Shen , Manman Lin , Jiafeng Jin , Wei Chen , Xiao Zhang , Chongxin Xu , Xiaodan Hu , Qing Zhu , Chengyu Chen , Yajing Xie , Ofentse Jacob Pooe , Neil Crickmore , Xianjin Liu , Peng Lü , Yuan Liu
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Abstract

Bacillus thuringiensis (Bt) Cry2Aa is a member of the Cry pore-forming, 3-domain, toxin family with activity against both lepidopteran and dipteran insects. Although domains II and III of the Cry toxins are believed to represent the primary specificity determinant through specific binding to cell receptors, it has been proposed that the pore-forming domain I of Cry2Aa also has such a role. Thus, a greater understanding of the functions of Cry2Aa’s different domains could potentially be helpful in the rational design of improved toxins.

In this work, cry2Aa and its domain fragments (DI, DII, DIII, DI-II and DII-DIII) were subcloned into the vector pGEX-6P-1 and expressed in Escherichia coli. Each protein was recognized by anti-Cry2Aa antibodies and, except for the DII fragment, could block binding of the antibody to Cry2Aa. Cry2Aa and its DI and DI-II fragments bound to brush border membrane vesicles (BBMV) from H. armigera and also to a ca 150 kDa BBMV protein on a far western (ligand) blot. In contrast the DII, DIII and DII-III fragments bound to neither of these. None of the fragments were stable in H. armigera gut juice nor showed any toxicity towards this insect. Our results indicate that contrary to the general model of Cry toxin activity domain I plays a role in the binding of the toxin to the insect midgut.

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苏云金芽孢杆菌 Cry2Aa 单个结构域的特征表明,结构域 I 可能是与 Helicoverpa armigera 的结合点。
苏云金芽孢杆菌(Bt)Cry2Aa 是具有 3 个结构域的 Cry 孔隙形成毒素家族的成员,对鳞翅目和双翅目昆虫都具有活性。尽管人们认为 Cry 毒素的结构域 II 和 III 是通过与细胞受体特异性结合来决定特异性的主要因素,但也有人认为 Cry2Aa 的孔形成结构域 I 也有这样的作用。因此,进一步了解 Cry2Aa 不同结构域的功能可能有助于合理设计改良毒素。在这项工作中,cry2Aa 及其结构域片段(DI、DII、DIII、DI-II 和 DII-DIII)被亚克隆到载体 pGEX-6P-1 中,并在大肠杆菌中表达。抗 Cry2Aa 抗体可识别每种蛋白质,除 DII 片段外,其他片段均可阻断抗体与 Cry2Aa 的结合。Cry2Aa 及其 DI 和 DI-II 片段与 H. armigera 的刷状缘膜囊泡 (BBMV) 结合,在远西(配体)印迹上还与约 150 kDa 的 BBMV 蛋白结合。与此相反,DII、DIII 和 DII-III 片段与上述两种蛋白都没有结合。这些片段在 H. armigera 肠液中都不稳定,对这种昆虫也没有任何毒性。我们的研究结果表明,与 Cry 毒素活性的一般模型相反,I 结构域在毒素与昆虫中肠的结合过程中发挥了作用。
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来源期刊
CiteScore
6.10
自引率
5.90%
发文量
94
审稿时长
1 months
期刊介绍: The Journal of Invertebrate Pathology presents original research articles and notes on the induction and pathogenesis of diseases of invertebrates, including the suppression of diseases in beneficial species, and the use of diseases in controlling undesirable species. In addition, the journal publishes the results of physiological, morphological, genetic, immunological and ecological studies as related to the etiologic agents of diseases of invertebrates. The Journal of Invertebrate Pathology is the adopted journal of the Society for Invertebrate Pathology, and is available to SIP members at a special reduced price.
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