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肠出血性大肠杆菌 T6SS 的核心蛋白及推定效应蛋白和免疫蛋白分析。

Analyses of Core Proteins and Putative Effector and Immunity Proteins for T6SS in Enterohemorrhagic .

机构信息

Department of Cell Biology, Centro de Investigación y de Estudios Avanzados del IPN (CINVESTAV-IPN), Mexico City, Mexico.

出版信息

Front Cell Infect Microbiol. 2020 May 5;10:195. doi: 10.3389/fcimb.2020.00195. eCollection 2020.

Abstract

Shiga-toxin-producing (STEC) has become an important pathogen that can cause diarrhea, hemorrhagic colitis and hemolytic uremic syndrome (HUS) in humans. Recent reports show that the type VI secretion system (T6SS) from EHEC is required to produce infection in a murine model and its expression has been related to a higher prevalence of HUS. In this work, we use bioinformatics analyses to identify the core genes of the T6SS and compared the differences between these components among the two published genomes for EHEC O157:H7 strain EDL933. Prototype strain EDL933 was further compared with other O157:H7 genomes. Unlike other typical T6SS effectors found in , we identified that there are several family genes in EHEC, which could serve as T6SS effectors. and PCR analyses of the differences between genes in the two existing genomes, allowed us to determine that the most recently published genome is more reliable to study the genes. Analyzing the putative tridimensional structure of Rhs proteins, as well as the motifs found in their C-terminal end, allowed us to predict their possible functions. A phylogenetic analysis showed that the orphan genes are more closely related between them than the genes belonging to islands and that they are divided into three clades. Analyses of the downstream region of the genes for identifying hypothetical immunity proteins showed that every gene has an associated small ORF (129-609 nucleotides). These genes could serve as immunity proteins as they had several interaction motifs as well as structural homology with other known immunity proteins. Our findings highlight the relevance of the T6SS in EHEC as well as the possible function of the Rhs effectors of EHEC O157:H7 during pathogenesis and bacterial competition, and the identification of novel effectors for the T6SS using a structural approach.

摘要

产志贺毒素(STEC)已成为一种重要的病原体,可导致人类腹泻、出血性结肠炎和溶血尿毒症综合征(HUS)。最近的报告表明,EHEC 的 VI 型分泌系统(T6SS)是在小鼠模型中产生感染所必需的,其表达与 HUS 的更高发生率有关。在这项工作中,我们使用生物信息学分析来鉴定 T6SS 的核心基因,并比较了在两个已发表的 EHEC O157:H7 菌株 EDL933 基因组之间这些成分的差异。原型菌株 EDL933 进一步与其他 O157:H7 基因组进行了比较。与其他典型的 T6SS 效应器不同,我们在 EHEC 中鉴定出有几个 家族基因,它们可以作为 T6SS 效应器。和 PCR 分析两个现有基因组中 基因的差异,使我们能够确定最近发表的基因组更适合研究 基因。分析 Rhs 蛋白的可能三维结构以及其 C 端末端发现的基序,使我们能够预测它们的可能功能。系统发育分析表明,孤儿 基因彼此之间比属于 岛的 基因更密切相关,并且它们分为三个分支。对 基因下游区域进行分析以识别假设的免疫蛋白,表明每个基因都有一个相关的小 ORF(129-609 个核苷酸)。这些基因可以作为免疫蛋白,因为它们具有几个相互作用基序,并且与其他已知的免疫蛋白具有结构同源性。我们的研究结果强调了 T6SS 在 EHEC 中的重要性,以及 EHEC O157:H7 中的 Rhs 效应器在发病机制和细菌竞争中的可能功能,以及使用结构方法鉴定 T6SS 的新型效应器。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/c422/7216683/5c5b98c41281/fcimb-10-00195-g0001.jpg

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