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AVR2 效应物通过效应物无序逃避 R2 识别。

The AVR2 Effector Escapes R2 Recognition Through Effector Disordering.

机构信息

Key Lab for Biopesticide and Chemical Biology, Ministry of Education, Fujian Agriculture and Forestry University, Fuzhou, China.

Fujian Key Laboratory of Plant Virology, Institute of Plant Virology, Fujian Agricultural and Forestry University, Fuzhou, Fujian 350002, China.

出版信息

Mol Plant Microbe Interact. 2020 Jul;33(7):921-931. doi: 10.1094/MPMI-07-19-0179-R. Epub 2020 Jun 1.

DOI:10.1094/MPMI-07-19-0179-R
PMID:32212906
Abstract

Intrinsic disorder is a common structural characteristic of proteins and a central player in the biochemical processes of species. However, the role of intrinsic disorder in the evolution of plant-pathogen interactions is rarely investigated. Here, we explored the role of intrinsic disorder in the development of the pathogenicity in the RXLR AVR2 effector of . We found AVR2 exhibited high nucleotide diversity generated by point mutation, early-termination, altered start codon, deletion/insertion, and intragenic recombination and is predicted to be an intrinsically disordered protein. AVR2 amino acid sequences conferring a virulent phenotype had a higher disorder tendency in both the N- and C-terminal regions compared with sequences conferring an avirulent phenotype. In addition, we also found virulent AVR2 mutants gained one or two short linear interaction motifs, the critical components of disordered proteins required for protein-protein interactions. Furthermore, virulent AVR2 mutants were predicted to be unstable and have a short protein half-life. Taken together, these results support the notion that intrinsic disorder is important for the effector function of pathogens and demonstrate that SLiM-mediated protein-protein interaction in the C-terminal effector domain might contribute greatly to the evasion of resistance-protein detection in .

摘要

内在无序是蛋白质的常见结构特征,也是物种生化过程的核心参与者。然而,内在无序在植物-病原体相互作用进化中的作用很少被研究。在这里,我们探讨了内在无序在. 的 RXLR AVR2 效应物致病性发展中的作用。我们发现 AVR2 表现出由点突变、早期终止、改变起始密码子、缺失/插入和基因内重组产生的高核苷酸多样性,并且预测为一种内在无序的蛋白质。与赋予无毒表型的序列相比,赋予毒性表型的 AVR2 氨基酸序列在 N-和 C-末端区域都具有更高的无序倾向。此外,我们还发现,毒性 AVR2 突变体获得了一个或两个短线性相互作用基序,这是无序蛋白质中用于蛋白质-蛋白质相互作用的关键组成部分。此外,毒性 AVR2 突变体被预测为不稳定的,并且蛋白质半衰期较短。综上所述,这些结果支持了内在无序对于病原体效应子功能很重要的观点,并表明 C 末端效应子结构域中 SLiM 介导的蛋白质-蛋白质相互作用可能极大地有助于逃避. 中抗性蛋白的检测。

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