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Cry 毒素在. 中利用多个 ATP 结合盒转运蛋白亚家族 C 成员作为低效率受体

Cry Toxins Use Multiple ATP-Binding Cassette Transporter Subfamily C Members as Low-Efficiency Receptors in .

机构信息

Graduate School of Bio-Applications and Systems Engineering, Tokyo University of Agriculture and Technology, 2-24-16 Koganei, Koganei 184-8588, Tokyo, Japan.

Japan Society for the Promotion of Science Research Fellowship for Young Scientists, 5-3-1 Kojimachi, Chiyoda-ku 102-0083, Tokyo, Japan.

出版信息

Biomolecules. 2024 Feb 23;14(3):271. doi: 10.3390/biom14030271.

Abstract

Recent studies have suggested that ABC transporters are the main receptors of Cry toxins. However, the receptors of many Cry toxins have not been identified. In this study, we used a heterologous cell expression system to identify ABC transporter subfamily C members (BmABCCs) that function as receptors for five Cry toxins active in Lepidopteran insects: Cry1Aa, Cry1Ca, Cry1Da, Cry8Ca, and Cry9Aa. All five Cry toxins can use multiple ABCCs as low-efficiency receptors, which induce cytotoxicity only at high concentrations. Surface plasmon resonance analysis revealed that the values between the toxins and BmABCC1 and BmABCC4 were 10 to 10 M, suggesting binding affinities 8- to 10,000-fold lower than those between Cry1Aa and BmABCC2, which are susceptibility-determining receptors for Cry1Aa. Bioassays in BmABCC-knockout silkworm strains showed that these low-efficiency receptors are not involved in sensitivity to Cry toxins. The findings suggest that each family of Cry toxins uses multiple BmABCCs as low-efficiency receptors in the insect midgut based on the promiscuous binding of their receptor-binding regions. Each Cry toxin seems to have evolved to utilize one or several ABC transporters as susceptibility-determining receptors.

摘要

最近的研究表明,ABC 转运蛋白是 Cry 毒素的主要受体。然而,许多 Cry 毒素的受体尚未被鉴定。在这项研究中,我们使用异源细胞表达系统来鉴定 ABC 转运蛋白亚家族 C 成员(BmABCCs),这些成员是五种对鳞翅目昆虫具有活性的 Cry 毒素的受体:Cry1Aa、Cry1Ca、Cry1Da、Cry8Ca 和 Cry9Aa。这五种 Cry 毒素都可以使用多个 ABCC 作为低效率受体,只有在高浓度下才会诱导细胞毒性。表面等离子体共振分析显示,毒素与 BmABCC1 和 BmABCC4 之间的 值在 10 到 10 M 之间,这表明结合亲和力比 Cry1Aa 与 BmABCC2 之间的结合亲和力低 8 到 10,000 倍,BmABCC2 是 Cry1Aa 的敏感性决定受体。在 BmABCC 敲除家蚕品系中的生物测定表明,这些低效率受体不参与对 Cry 毒素的敏感性。这些发现表明,每种 Cry 毒素家族都基于其受体结合区域的混杂结合,将多个 BmABCC 作为低效率受体在昆虫中肠中使用。每种 Cry 毒素似乎都进化为利用一种或几种 ABC 转运蛋白作为敏感性决定受体。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/b423/10968512/6ef1a2e96db4/biomolecules-14-00271-g001.jpg

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