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一种毒素结合钙黏蛋白的片段增强苏云金芽孢杆菌Cry1A毒素的杀虫活性与寡聚体形成相关。

Enhancement of insecticidal activity of Bacillus thuringiensis Cry1A toxins by fragments of a toxin-binding cadherin correlates with oligomer formation.

作者信息

Pacheco Sabino, Gómez Isabel, Gill Sarjeet S, Bravo Alejandra, Soberón Mario

机构信息

Instituto de Biotecnología, Universidad Nacional Autónoma de México, Apdo. Postal 510-3, Cuernavaca, Morelos 62250, Mexico.

出版信息

Peptides. 2009 Mar;30(3):583-8. doi: 10.1016/j.peptides.2008.08.006. Epub 2008 Aug 20.

DOI:10.1016/j.peptides.2008.08.006
PMID:18778745
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC2693380/
Abstract

Cry1A toxins produced by Bacillus thuringiensis bind a cadherin receptor that mediates toxicity in different lepidopteran insect larvae. Insect cadherin receptors are modular proteins composed of three domains, the ectodomain formed by 9-12 cadherin repeats (CR), the transmembrane domain and the intracellular domain. Cry1A toxins interact with three regions of the Manduca sexta cadherin receptor that are located in CR7, CR11 and CR12 cadherin repeats. Binding of Cry1A toxin to cadherin induces oligomerization of the toxin, which is essential for membrane insertion. Also, it has been reported that cadherin fragments containing the CR12 region enhanced the insecticidal activity of Cry1Ab toxin to M. sexta and other lepidopteran larvae. Here we report that cadherin fragments corresponding to CR7 and CR11 regions also enhanced the activity of Cry1Ac and Cry1Ab toxin to M. sexta larvae, although not as efficient as the CR12 fragment. A single point mutation in the CR12 region (I1422R) affected Cry1Ac and Cry1Ab binding to the cadherin fragments and did not enhance the activity of Cry1Ab or Cry1Ac toxin in bioassays. Analysis of Cry1Ab in vitro oligomer formation in the presence of wild type and mutated cadherin fragments showed a correlation between enhancement of Cry1A toxin activity in bioassays and in vitro Cry1Ab-oligomer formation. Our data shows that formation of Cry1A toxin oligomer is in part responsible for the enhancement of Cry1A toxicity by cadherin fragments that is observed in vivo.

摘要

苏云金芽孢杆菌产生的Cry1A毒素可结合一种钙黏蛋白受体,该受体介导对不同鳞翅目昆虫幼虫的毒性作用。昆虫钙黏蛋白受体是由三个结构域组成的模块化蛋白质,即由9 - 12个钙黏蛋白重复序列(CR)形成的胞外结构域、跨膜结构域和胞内结构域。Cry1A毒素与烟草天蛾钙黏蛋白受体位于CR7、CR11和CR12钙黏蛋白重复序列中的三个区域相互作用。Cry1A毒素与钙黏蛋白的结合会诱导毒素寡聚化,这对于膜插入至关重要。此外,据报道,含有CR12区域的钙黏蛋白片段增强了Cry1Ab毒素对烟草天蛾和其他鳞翅目幼虫的杀虫活性。在此我们报道,对应于CR7和CR11区域的钙黏蛋白片段也增强了Cry1Ac和Cry1Ab毒素对烟草天蛾幼虫的活性,尽管不如CR12片段有效。CR12区域的一个单点突变(I1422R)影响了Cry1Ac和Cry1Ab与钙黏蛋白片段的结合,并且在生物测定中未增强Cry1Ab或Cry1Ac毒素的活性。在存在野生型和突变型钙黏蛋白片段的情况下对Cry1Ab体外寡聚体形成的分析表明,生物测定中Cry1A毒素活性的增强与体外Cry1Ab - 寡聚体形成之间存在相关性。我们的数据表明,Cry1A毒素寡聚体的形成部分导致了在体内观察到的钙黏蛋白片段增强Cry1A毒性的现象。

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