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cAMP 受体样蛋白 CLP 是一种新型的 c-di-GMP 受体,可将细胞间信号传递与黄单胞菌毒力基因表达联系起来。

The cAMP receptor-like protein CLP is a novel c-di-GMP receptor linking cell-cell signaling to virulence gene expression in Xanthomonas campestris.

机构信息

Institute of Biochemistry, National Chung-Hsing University, Taichung 40227, Taiwan, ROC.

出版信息

J Mol Biol. 2010 Feb 26;396(3):646-62. doi: 10.1016/j.jmb.2009.11.076. Epub 2009 Dec 18.

DOI:10.1016/j.jmb.2009.11.076
PMID:20004667
Abstract

Cyclic-di-GMP [bis-(3'-5')-cyclic diguanosine monophosphate] controls a wide range of functions in eubacteria, yet little is known about the underlying regulatory mechanisms. In the plant pathogen Xanthomonas campestris, expression of a subset of virulence genes is regulated by c-di-GMP and also by the CAP (catabolite activation protein)-like protein XcCLP, a global regulator in the CRP/FNR superfamily. Here, we report structural and functional insights into the interplay between XcCLP and c-di-GMP in regulation of gene expression. XcCLP bound target promoter DNA with submicromolar affinity in the absence of any ligand. This DNA-binding capability was abrogated by c-di-GMP, which bound to XcCLP with micromolar affinity. The crystal structure of XcCLP showed that the protein adopted an intrinsically active conformation for DNA binding. Alteration of residues of XcCLP implicated in c-di-GMP binding through modeling studies caused a substantial reduction in binding affinity for the nucleotide and rendered DNA binding by these variant proteins insensitive to inhibition by c-di-GMP. Together, these findings reveal the structural mechanism behind a novel class of c-di-GMP effector proteins in the CRP/FNR superfamily and indicate that XcCLP regulates bacterial virulence gene expression in a manner negatively controlled by the c-di-GMP concentrations.

摘要

环二鸟苷酸 [双-(3'-5')-环鸟苷酸单磷酸] 控制着真细菌的广泛功能,但对于潜在的调节机制知之甚少。在植物病原菌黄单胞菌中,一组毒力基因的表达受 c-di-GMP 以及 CAP(分解代谢物激活蛋白)样蛋白 XcCLP 调控,后者是 CRP/FNR 超家族中的全局调控因子。在这里,我们报告了 XcCLP 和 c-di-GMP 之间相互作用的结构和功能见解,以调节基因表达。在没有任何配体的情况下,XcCLP 以亚微摩尔亲和力结合靶启动子 DNA。这种 DNA 结合能力被 c-di-GMP 所破坏,c-di-GMP 以微摩尔亲和力与 XcCLP 结合。XcCLP 的晶体结构表明,该蛋白采用固有活性构象进行 DNA 结合。通过建模研究改变 XcCLP 中与 c-di-GMP 结合相关的残基,导致与核苷酸的结合亲和力大大降低,并且这些变异蛋白的 DNA 结合对 c-di-GMP 的抑制作用不敏感。总之,这些发现揭示了 CRP/FNR 超家族中新一类 c-di-GMP 效应蛋白的结构机制,并表明 XcCLP 以 c-di-GMP 浓度负调控的方式调节细菌毒力基因表达。

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