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控制毒力调节蛋白的不同单一氨基酸替换对链球菌发病机制有不同影响。

Distinct single amino acid replacements in the control of virulence regulator protein differentially impact streptococcal pathogenesis.

机构信息

Department of Biochemistry and Molecular Biology, MD Anderson Cancer Center, Houston, Texas, United States of America.

出版信息

PLoS Pathog. 2011 Oct;7(10):e1002311. doi: 10.1371/journal.ppat.1002311. Epub 2011 Oct 20.

Abstract

Sequencing of invasive strains of group A streptococci (GAS) has revealed a diverse array of single nucleotide polymorphisms in the gene encoding the control of virulence regulator (CovR) protein. However, there is limited information regarding the molecular mechanisms by which CovR single amino acid replacements impact GAS pathogenesis. The crystal structure of the CovR C-terminal DNA-binding domain was determined to 1.50 Å resolution and revealed a three-stranded β-sheet followed by a winged helix-turn-helix DNA binding motif. Modeling of the CovR protein-DNA complex indicated that CovR single amino acid replacements observed in clinical GAS isolates could directly alter protein-DNA interaction and impact protein structure. Isoallelic GAS strains that varied by a single amino acid replacement in the CovR DNA binding domain had significantly different transcriptomes compared to wild-type and to each other. Similarly, distinct recombinant CovR variants had differential binding affinity for DNA from the promoter regions of several virulence factor-encoding genes. Finally, mice that were challenged with GAS CovR isoallelic strains had significantly different survival times, which correlated with the transcriptome and protein-DNA binding studies. Taken together, these data provide structural and functional insights into the critical and distinct effects of variation in the CovR protein on GAS pathogenesis.

摘要

对侵袭性 A 组链球菌(GAS)菌株进行测序,揭示了编码毒力调节蛋白(CovR)的基因中存在大量单核苷酸多态性。然而,关于 CovR 单个氨基酸替换如何影响 GAS 发病机制的分子机制的信息有限。CovR C 末端 DNA 结合域的晶体结构已确定为 1.50 Å 分辨率,并显示出三股β-折叠,其后是带有翼状螺旋-转角-螺旋 DNA 结合基序。CovR 蛋白-DNA 复合物的建模表明,在临床 GAS 分离株中观察到的 CovR 单个氨基酸替换可能直接改变蛋白-DNA 相互作用并影响蛋白结构。与野生型和彼此相比,在 CovR DNA 结合域中单个氨基酸替换不同的同效等位基因 GAS 菌株的转录组有显著差异。同样,不同的重组 CovR 变体对来自几种毒力因子编码基因启动子区域的 DNA 的结合亲和力也不同。最后,用 GAS CovR 同效等位基因菌株进行挑战的小鼠的存活时间有显著差异,这与转录组和蛋白-DNA 结合研究相关。总之,这些数据提供了结构和功能方面的见解,阐明了 CovR 蛋白变异对 GAS 发病机制的关键和独特影响。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/9fc3/3197619/bf54a77cd2c0/ppat.1002311.g001.jpg

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