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本文引用的文献

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Characterization of the RofA regulon in the pandemic M1 and emergent M1 lineages of .大流行 M1 株和新兴 M1 株中 RofA 调控子的特性研究。
Microb Genom. 2023 Dec;9(12). doi: 10.1099/mgen.0.001159.
2
A novel RofA-family transcriptional regulator, GadR, controls the development of acid resistance in .一种新型的 RofA 家族转录调节因子 GadR 控制耐酸性的发育。
mBio. 2023 Dec 19;14(6):e0171623. doi: 10.1128/mbio.01716-23. Epub 2023 Oct 26.
3
Glucose levels affect MgaSpn regulation on the virulence and adaptability of Streptococcus pneumoniae.葡萄糖水平影响MgaSpn对肺炎链球菌毒力和适应性的调控。
Microb Pathog. 2023 Jan;174:105896. doi: 10.1016/j.micpath.2022.105896. Epub 2022 Nov 29.
4
Pilus proteins from Streptococcus pyogenes stimulate innate immune responses through Toll-like receptor 2.化脓链球菌的菌毛蛋白通过 Toll 样受体 2 刺激固有免疫反应。
Immunol Cell Biol. 2022 Mar;100(3):174-185. doi: 10.1111/imcb.12523. Epub 2022 Feb 24.
5
PRD-Containing Virulence Regulators (PCVRs) in Pathogenic Bacteria.致病菌中的含 PRD 结构域的毒力调节蛋白(PCVRs)
Front Cell Infect Microbiol. 2021 Oct 19;11:772874. doi: 10.3389/fcimb.2021.772874. eCollection 2021.
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Genetics, Structure, and Function of Group A Streptococcal Pili.A组链球菌菌毛的遗传学、结构与功能
Front Microbiol. 2021 Feb 9;12:616508. doi: 10.3389/fmicb.2021.616508. eCollection 2021.
7
Phosphotransferase System Uptake and Metabolism of the β-Glucoside Salicin Impact Group A Streptococcal Bloodstream Survival and Soft Tissue Infection.磷酸转移酶系统摄取和β-糖苷柳醇的代谢影响 A 组链球菌血流生存和软组织感染。
Infect Immun. 2020 Sep 18;88(10). doi: 10.1128/IAI.00346-20.
8
Assays to Analyze Adhesion of Group A Streptococcus to Host Cells.分析 A 组链球菌黏附宿主细胞的检测方法。
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9
Influence of the phosphoenolpyruvate:carbohydrate phosphotransferase system on toxin gene expression and virulence in Bacillus anthracis.磷酸烯醇丙酮酸:碳水化合物磷酸转移酶系统对炭疽芽孢杆菌毒素基因表达和毒力的影响。
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10
Graph-based genome alignment and genotyping with HISAT2 and HISAT-genotype.基于图的基因组比对和基因分型与 HISAT2 和 HISAT-genotype。
Nat Biotechnol. 2019 Aug;37(8):907-915. doi: 10.1038/s41587-019-0201-4. Epub 2019 Aug 2.

独立调控因子 RofA 表现出含 PRD 结构域的毒力调控因子的特征。

The stand-alone regulator RofA exhibits characteristics of a PRD-containing virulence regulator.

机构信息

Department of Cell Biology and Molecular Genetics, Maryland Pathogen Research Institute, College Park, Maryland, USA.

Center for Bioinformatics and Computational Biology, University of Maryland, College Park, Maryland, USA.

出版信息

Infect Immun. 2024 Jun 11;92(6):e0008324. doi: 10.1128/iai.00083-24. Epub 2024 May 7.

DOI:10.1128/iai.00083-24
PMID:38712951
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC11237776/
Abstract

[group A streptococcus (GAS)] is a human pathogen capable of infecting diverse tissues. To successfully infect these sites, GAS must detect available nutrients and adapt accordingly. The phosphoenolpyruvate transferase system (PTS) mediates carbohydrate uptake and metabolic gene regulation to adapt to the nutritional environment. Regulation by the PTS can occur through phosphorylation of transcriptional regulators at conserved PTS-regulatory domains (PRDs). GAS has several PRD-containing stand-alone regulators with regulons encoding both metabolic genes and virulence factors [PRD-containing virulence regulators (PCVRs)]. One is RofA, which regulates the expression of virulence genes in multiple GAS serotypes. It was hypothesized that RofA is phosphorylated by the PTS in response to carbohydrate levels to coordinate virulence gene expression. In this study, the RofA regulon of M1T1 strain 5448 was determined using RNA sequencing. Two operons were consistently differentially expressed across growth in the absence of RofA; the pilus operon was downregulated, and the capsule operon was upregulated. This correlated with increased capsule production and decreased adherence to keratinocytes. Purified RofA-His was phosphorylated by PTS proteins EI and HPr, and phosphorylated RofA-FLAG was detected when GAS was grown in low-glucose C medium. Phosphorylated RofA was not observed when C medium was supplemented 10-fold with glucose. Mutations of select histidine residues within the putative PRDs contributed to the phosphorylation of RofA, although phosphorylation of RofA was still observed, suggesting other phosphorylation sites exist in the protein. Together, these findings support the hypothesis that RofA is a PCVR that may couple sugar metabolism with virulence regulation.

摘要

[A 组链球菌 (GAS)]是一种能够感染多种组织的人类病原体。为了成功感染这些部位,GAS 必须检测到可用的营养物质并相应地进行适应。磷酸烯醇丙酮酸转移酶系统 (PTS) 介导碳水化合物的摄取和代谢基因的调节,以适应营养环境。PTS 的调节可以通过在保守的 PTS 调节结构域 (PRD) 上磷酸化转录调节因子来实现。GAS 有几个包含 PRD 的独立调节因子,其调节子编码代谢基因和毒力因子[包含 PRD 的毒力调节因子 (PCVRs)]。其中一个是 RofA,它调节多种 GAS 血清型的毒力基因表达。据推测,RofA 会根据碳水化合物水平被 PTS 磷酸化,以协调毒力基因表达。在这项研究中,使用 RNA 测序确定了 M1T1 株 5448 的 RofA 调节子。在没有 RofA 的情况下,两个操纵子在生长过程中始终表现出差异表达;菌毛操纵子下调,荚膜操纵子上调。这与荚膜产量增加和角化细胞粘附减少相关。纯化的 RofA-His 被 PTS 蛋白 EI 和 HPr 磷酸化,当 GAS 在低葡萄糖 C 培养基中生长时,检测到磷酸化的 RofA-FLAG。当 C 培养基中葡萄糖补充 10 倍时,未观察到磷酸化的 RofA。在假定的 PRD 内选择组氨酸残基的突变有助于 RofA 的磷酸化,尽管仍观察到 RofA 的磷酸化,这表明该蛋白中存在其他磷酸化位点。总之,这些发现支持 RofA 是一种 PCVR 的假设,它可能将糖代谢与毒力调节偶联起来。