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表明, 类 VII 型分泌系统具有极高的遗传多样性,可能在细菌拮抗中发挥作用。

Extreme genetic diversity in the type VII secretion system of suggests a role in bacterial antagonism.

机构信息

Microbes in Health and Disease Theme, Newcastle University Biosciences Institute, Newcastle University, Newcastle upon Tyne, NE2 4HH, UK.

出版信息

Microbiology (Reading). 2021 Mar;167(3). doi: 10.1099/mic.0.001034. Epub 2021 Feb 18.

Abstract

The type VII protein secretion system (T7SS) has been characterized in members of the phyla Actinobacteria and Firmicutes. In mycobacteria the T7SS is intimately linked with pathogenesis and intracellular survival, while in Firmicutes there is mounting evidence that the system plays a key role in interbacterial competition. A conserved membrane-bound ATPase protein, termed EssC in , is a critical component of the T7SS and is the primary receptor for substrate proteins. Genetic diversity in the gene of has previously been reported, resulting in four protein variants that are linked to specific subsets of substrates. Here we have analysed the genetic diversity of the T7SS-encoding genes and substrate proteins across genome sequences. We find that there are seven EssC variants across the species that differ in their C-terminal region; each variant is correlated with a distinct subset of genes for likely substrate and accessory proteins. EssC1 is most common and is exclusively linked with polymorphic toxins harbouring a YeeF domain, whereas EssC5, EssC6 and EssC7 variants all code for an LXG domain protein adjacent to . Some variant strains encode an additional, truncated at their T7 gene cluster. The truncated EssC, comprising only the C-terminal half of the protein, matches the sequence of either EssC2, EssC3 or EssC4. In each case the truncated gene directly precedes a cluster of substrate/accessory protein genes acquired from the corresponding strain. Across strains we identified 40 LXG domain proteins, most of which are encoded at conserved genomic loci. These loci also harbour genes encoding immunity proteins and sometimes additional toxin fragments. Collectively our findings strongly suggest that the T7SS plays an important role in bacterial antagonism in this species.

摘要

VII 型蛋白分泌系统(T7SS)在放线菌门和厚壁菌门的成员中得到了描述。在分枝杆菌中,T7SS 与发病机制和细胞内生存密切相关,而在厚壁菌门中,越来越多的证据表明该系统在细菌间竞争中起着关键作用。一种保守的膜结合 ATP 酶蛋白,在 中称为 EssC,是 T7SS 的关键组成部分,也是底物蛋白的主要受体。 先前已经报道了 基因的遗传多样性,导致了四种与特定底物亚群相关的蛋白质变体。在这里,我们分析了 across 基因组序列中 T7SS 编码基因和底物蛋白的遗传多样性。我们发现该物种中有七种 EssC 变体,它们在 C 末端区域存在差异;每种变体都与一组特定的底物和辅助蛋白基因相关。EssC1 最为常见,仅与携带 YeeF 结构域的多态性毒素相关,而 EssC5、EssC6 和 EssC7 变体都编码一个相邻的 LXG 结构域蛋白 。一些 变体菌株在其 T7 基因簇处编码一个额外的截断 。截断的 EssC 仅包含蛋白质的 C 末端一半,与 EssC2、EssC3 或 EssC4 的序列匹配。在每种情况下,截断的基因直接位于从相应菌株获得的一组底物/辅助蛋白基因之前。在 across 株系中,我们鉴定了 40 种 LXG 结构域蛋白,其中大多数在保守的基因组基因座中编码。这些基因座还编码免疫蛋白基因,有时还有其他毒素片段。总的来说,我们的研究结果强烈表明 T7SS 在该物种的细菌拮抗作用中起着重要作用。

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