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共栖噬菌体元件的协调支持细菌-噬菌体的合作。

Coordination of cohabiting phage elements supports bacteria-phage cooperation.

机构信息

The School of Molecular Cell Biology and Biotechnology, Faculty of Life Sciences, Tel Aviv University, Ramat Aviv, Tel Aviv, 69978, Israel.

出版信息

Nat Commun. 2019 Nov 21;10(1):5288. doi: 10.1038/s41467-019-13296-x.

Abstract

Bacterial pathogens often carry multiple prophages and other phage-derived elements within their genome, some of which can produce viral particles in response to stress. Listeria monocytogenes 10403S harbors two phage elements in its chromosome, both of which can trigger bacterial lysis under stress: an active prophage (ϕ10403S) that promotes the virulence of its host and can produce infective virions, and a locus encoding phage tail-like bacteriocins. Here, we show that the two phage elements are co-regulated, with the bacteriocin locus controlling the induction of the prophage and thus its activity as a virulence-associated molecular switch. More specifically, a metalloprotease encoded in the bacteriocin locus is upregulated in response to stress and acts as an anti-repressor for CI-like repressors encoded in each phage element. Our results provide molecular insight into the phenomenon of polylysogeny and its intricate adaptation to complex environments.

摘要

细菌病原体的基因组中常常携带多个噬菌体和其他噬菌体衍生元件,其中一些在受到压力时可以产生病毒颗粒。单核细胞增生李斯特菌 10403S 在其染色体中携带两个噬菌体元件,它们都可以在压力下触发细菌裂解:一个活跃的噬菌体(ϕ10403S)促进宿主的毒力并能产生感染性病毒粒子,以及一个编码噬菌体尾部细菌素的基因座。在这里,我们表明这两个噬菌体元件是共同调节的,细菌素基因座控制着噬菌体的诱导及其作为与毒力相关的分子开关的活性。更具体地说,细菌素基因座中编码的金属蛋白酶在受到压力时上调,并作为每个噬菌体元件中编码的 CI 样阻遏物的反阻遏物发挥作用。我们的结果为多溶源性现象及其对复杂环境的复杂适应提供了分子见解。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/2bb9/6872733/02f428c7b259/41467_2019_13296_Fig1_HTML.jpg

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