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巴尔通体中VirB/D4型IV型分泌系统的三次独立获得所揭示的致病适应的进化动力学

Evolutionary Dynamics of Pathoadaptation Revealed by Three Independent Acquisitions of the VirB/D4 Type IV Secretion System in Bartonella.

作者信息

Harms Alexander, Segers Francisca H I D, Quebatte Maxime, Mistl Claudia, Manfredi Pablo, Körner Jonas, Chomel Bruno B, Kosoy Michael, Maruyama Soichi, Engel Philipp, Dehio Christoph

机构信息

Focal Area Infection Biology, Biozentrum, University of Basel, Switzerland.

Department of Fundamental Microbiology, University of Lausanne, Switzerland.

出版信息

Genome Biol Evol. 2017 Mar 1;9(3):761-776. doi: 10.1093/gbe/evx042.

Abstract

The α-proteobacterial genus Bartonella comprises a group of ubiquitous mammalian pathogens that are studied as a model for the evolution of bacterial pathogenesis. Vast abundance of two particular phylogenetic lineages of Bartonella had been linked to enhanced host adaptability enabled by lineage-specific acquisition of a VirB/D4 type IV secretion system (T4SS) and parallel evolution of complex effector repertoires. However, the limited availability of genome sequences from one of those lineages as well as other, remote branches of Bartonella has so far hampered comprehensive understanding of how the VirB/D4 T4SS and its effectors called Beps have shaped Bartonella evolution. Here, we report the discovery of a third repertoire of Beps associated with the VirB/D4 T4SS of B. ancashensis, a novel human pathogen that lacks any signs of host adaptability and is only distantly related to the two species-rich lineages encoding a VirB/D4 T4SS. Furthermore, sequencing of ten new Bartonella isolates from under-sampled lineages enabled combined in silico analyses and wet lab experiments that suggest several parallel layers of functional diversification during evolution of the three Bep repertoires from a single ancestral effector. Our analyses show that the Beps of B. ancashensis share many features with the two other repertoires, but may represent a more ancestral state that has not yet unleashed the adaptive potential of such an effector set. We anticipate that the effectors of B. ancashensis will enable future studies to dissect the evolutionary history of Bartonella effectors and help unraveling the evolutionary forces underlying bacterial host adaptation.

摘要

α-变形菌属巴尔通体包含一组普遍存在的哺乳动物病原体,它们被作为细菌致病机制进化的模型进行研究。巴尔通体的两个特定系统发育谱系的大量存在与通过谱系特异性获得VirB/D4型IV分泌系统(T4SS)和复杂效应子库的平行进化所实现的增强宿主适应性有关。然而,到目前为止,来自这些谱系之一以及巴尔通体其他较远分支的基因组序列可用性有限,阻碍了对VirB/D4 T4SS及其效应子Beps如何塑造巴尔通体进化的全面理解。在这里,我们报告发现了与安卡申斯巴尔通体的VirB/D4 T4SS相关的第三组Beps,安卡申斯巴尔通体是一种新型人类病原体,缺乏任何宿主适应性迹象,并且与编码VirB/D4 T4SS的两个物种丰富的谱系关系甚远。此外,对来自采样不足谱系的十个新巴尔通体分离株进行测序,使得能够进行计算机分析和湿实验室实验相结合的研究,这些研究表明,在从单个祖先效应子进化出三组Beps的过程中存在几个平行的功能多样化层次。我们的分析表明,安卡申斯巴尔通体的Beps与其他两组Beps有许多共同特征,但可能代表一种尚未释放此类效应子集适应性潜力的更原始状态。我们预计,安卡申斯巴尔通体的效应子将使未来的研究能够剖析巴尔通体效应子的进化历史,并有助于揭示细菌宿主适应背后的进化力量。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/49ab/5381568/fbcbe4911a35/evx042f1p.jpg

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