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通过转录组和 ChIP-exo 分析破译 GntR 家族调控因子的调控网络及其对柑橘溃疡病菌毒力的贡献。

Deciphering the regulon of a GntR family regulator via transcriptome and ChIP-exo analyses and its contribution to virulence in Xanthomonas citri.

机构信息

Citrus Research and Education Center, Department of Microbiology and Cell Science, IFAS, University of Florida, 700 Experiment Station Road, Lake Alfred, FL, 33850, USA.

出版信息

Mol Plant Pathol. 2017 Feb;18(2):249-262. doi: 10.1111/mpp.12397. Epub 2016 Jul 22.

Abstract

Xanthomonas contains a large group of plant-associated species, many of which cause severe diseases on important crops worldwide. Six gluconate-operon repressor (GntR) family transcriptional regulators are predicted in Xanthomonas, one of which, belonging to the YtrA subfamily, plays a prominent role in bacterial virulence. However, the direct targets and comprehensive regulatory profile of YtrA remain unknown. Here, we performed microarray and high-resolution chromatin immunoprecipitation-exonuclease (ChIP-exo) experiments to identify YtrA direct targets and its DNA binding motif in X. citri ssp. citri (Xac), the causal agent of citrus canker. Integrative microarray and ChIP-exo data analysis revealed that YtrA directly regulates three operons by binding to a palindromic motif GGTG-N -CACC at the promoter region. A similar palindromic motif and YtrA homologues were also identified in many other bacteria, including Stenotrophomonas, Pseudoxanthomonas and Frateuria, indicating a widespread phenomenon. Deletion of ytrA in Xac abolishes bacterial virulence and induction of the hypersensitive response (HR). We found that YtrA regulates the expression of hrp/hrc genes encoding the bacterial type III secretion system (T3SS) and controls multiple biological processes, including motility and adhesion, oxidative stress, extracellular enzyme production and iron uptake. YtrA represses the expression of its direct targets in artificial medium or in planta. Importantly, over-expression of yro3, one of the YtrA directly regulated operons which contains trmL and XAC0231, induced weaker canker symptoms and down-regulation of hrp/hrc gene expression, suggesting a negative regulation in Xac virulence and T3SS. Our study has significantly advanced the mechanistic understanding of YtrA regulation and its contribution to bacterial virulence.

摘要

黄单胞菌包含一大组与植物相关的物种,其中许多在全球范围内对重要作物造成严重疾病。预测黄单胞菌中有六个葡萄糖酸盐操纵子阻遏物(GntR)家族转录调节剂,其中一个属于 YtrA 亚家族,在细菌毒力中起着重要作用。然而,YtrA 的直接靶标和综合调控谱尚不清楚。在这里,我们进行了微阵列和高分辨率染色质免疫沉淀-外切酶(ChIP-exo)实验,以确定 X. citri ssp. citri(Xac)中 YtrA 的直接靶标及其 DNA 结合基序,Xac 是柑橘溃疡病的病原体。整合微阵列和 ChIP-exo 数据分析表明,YtrA 通过在启动子区域结合回文基序 GGTG-N-CACC 直接调节三个操纵子。在许多其他细菌中,包括 Stenotrophomonas、Pseudoxanthomonas 和 Frateuria,也发现了类似的回文基序和 YtrA 同源物,这表明这是一种广泛存在的现象。Xac 中 ytrA 的缺失会消除细菌的毒力和诱导过敏反应(HR)。我们发现 YtrA 调节编码细菌 III 型分泌系统(T3SS)的 hrp/hrc 基因的表达,并控制多种生物学过程,包括运动性和粘附性、氧化应激、胞外酶产生和铁摄取。YtrA 在人工培养基或植物中抑制其直接靶标的表达。重要的是,YtrA 直接调控的操纵子之一 yro3 的过表达,其中包含 trmL 和 XAC0231,诱导较弱的溃疡症状和下调 hrp/hrc 基因表达,表明在 Xac 毒力和 T3SS 中存在负调控。我们的研究显著推进了对 YtrA 调节及其对细菌毒力贡献的机制理解。

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