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Deep-sea vent ε-proteobacterial genomes provide insights into emergence of pathogens

机译:深海通风的ε-细菌基因组可洞察病原体的出现

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Deep-sea vents are the light-independent, highly productive ecosystems driven primarily by chemolithoautotrophic microorganisms, in particular by ε-Proteobacteria phylogenetically related to important pathogens. We analyzed genomes of two deep-sea vent ε-Proteobacteria strains, Sulfurovum sp. NBC37-1 and Nitratiruptor sp. SB155-2, which provide insights not only into their unusual niche on the seafloor, but also into the origins of virulence in their pathogenic relatives, Helicobacter and Campylobacter species. The deep-sea vent ε-proteobacterial genomes encode for multiple systems for respiration, sensing and responding to environment, and detoxifying heavy metals, reflecting their adaptation to the deep-sea vent environment. Although they are nonpathogenic, both deep-sea vent ε-Proteobacteria share many virulence genes with pathogenic ε-Proteobacteria, including genes for virulence factor MviN, hemolysin, invasion antigen CiaB, and the N-linked glycosylation gene cluster. In addition, some virulence determinants (such as the H_2-uptake hydrogenase) and genomic plasticity of the pathogenic descendants appear to have roots in deep-sea vent ε-Proteobacteria. These provide ecological advantages for hydrothermal vent ε-Proteobacteria who thrive in their deep-sea habitat and are essential for both the efficient colonization and persistent infections of their pathogenic relatives. Our comparative genomic analysis suggests that there are previously unrecognized evolutionary links between important human/animal pathogens and their nonpathogenic, symbiotic, chemolithoautotrophic deep-sea relatives.
机译:深海通风口是不依赖光的,高产的生态系统,主要由化石自养微生物驱动,特别是与重要病原体发生系统发育关系的ε-Proteobacteria。我们分析了两个深海通风ε-变形杆菌菌株Sulfurovum sp。的基因组。 NBC37-1和Nitratiruptor sp。 SB155-2,不仅为他们在海底上的不寻常生态位提供了见识,而且还为他们的致病亲戚,幽门螺杆菌和弯曲杆菌种的毒力起源提供了见识。深海通风口ε-细菌基因组编码多种系统,用于呼吸,感知和响应环境以及对重金属进行解毒,从而反映了它们对深海通风口环境的适应性。尽管它们是非致病性的,但两种深海通风的ε-变形杆菌都与致病性ε-变形杆菌共享许多毒力基因,包括毒力因子MviN,溶血素,入侵抗原CiaB和N-连锁糖基化基因簇的基因。此外,某些毒力决定因素(例如H_2摄取氢化酶)和致病后代的基因组可塑性似乎起源于深海喷发ε-变形杆菌。这些为在深海栖息地繁衍生息的热液喷发ε-变形杆菌提供了生态优势,对于其病原体的有效定植和持续感染都是必不可少的。我们的比较基因组分析表明,重要的人类/动物病原体与其非致病性,共生性,化石营养自养型深海亲属之间以前没有公认的进化联系。

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