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Killing with proficiency: Integrated post-translational regulation of an offensive Type VI secretion system

机译:熟练熟练杀害:综合翻译后的vi分泌系统的翻译后调节

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The Type VI secretion system (T6SS) is widely used by bacterial pathogens as an effective weapon against bacterial competitors and is also deployed against host eukaryotic cells in some cases. It is a contractile nanomachine which delivers toxic effector proteins directly into target cells by dynamic cycles of assembly and firing. Bacterial cells adopt distinct post-translational regulatory strategies for deployment of the T6SS. ‘Defensive’ T6SSs assemble and fire in response to incoming attacks from aggressive neighbouring cells, and can utilise the Threonine Protein Phosphorylation (TPP) regulatory pathway to achieve this control. However, many T6SSs are ‘offensive’, firing at all-comers without the need for incoming attack or other cell contact-dependent signal. Post-translational control of the offensive mode has been less well defined but can utilise components of the same TPP pathway. Here, we used the anti-bacterial T6SS of Serratia marcescens to elucidate post-translational regulation of offensive T6SS deployment, using single-cell microscopy and genetic analyses. We show that the integration of the TPP pathway with the negative regulator TagF to control core T6SS machine assembly is conserved between offensive and defensive T6SSs. Signal-dependent PpkA-mediated phosphorylation of Fha is required to overcome inhibition of membrane complex assembly by TagF, whilst PppA-mediated dephosphorylation promotes spatial reorientation and efficient killing. In contrast, the upstream input of the TPP pathway defines regulatory strategy, with a new periplasmic regulator, RtkS, shown to interact with the PpkA kinase in S. marcescens. We propose a model whereby the opposing actions of the TPP pathway and TagF impose a delay on T6SS re-assembly after firing, providing an opportunity for spatial re-orientation of the T6SS in order to maximise the efficiency of competitor cell targeting. Our findings provide a better understanding of how bacterial cells deploy competitive weapons effectively, with implications for the structure and dynamics of varied polymicrobial communities.
机译:vI型分泌系统(T6SS)被细菌病原体广泛使用,作为针对细菌竞争机的有效武器,并且在某些情况下也将针对宿主真核细胞部署。它是一种收缩纳米载荷,通过组装和烧制的动态循环,将毒性效应蛋白直接输送到靶细胞中。细菌细胞采用不同的翻译后监管策略,用于部署T6SS。 ‘防御’ T6SSS响应于来自侵略性相邻细胞的进入攻击而组装和火灾,并且可以利用苏氨酸蛋白磷酸化(TPP)调节途径来实现这种对照。但是,许多T6SS都是‘攻击性和#x02019;,在所有clcers下射击,无需传入攻击或其他单元接触依赖信。令人反感模式的翻译后控制已经不太明确,但可以利用相同TPP通路的组件。在这里,我们使用单细胞显微镜和遗传分析来阐明Serratia Marcescens的抗菌T6SS来阐明进攻T6SS部署的翻译后调节。我们表明,TPP通路与负压器TAGF的集成控制核心T6SS机器组件在冒犯性和防御T6SS之间保守。信号依赖性的PPKA介导的FHA磷酸化需要克服TAGF的膜复合物组件的抑制,而PPPA介导的去磷酸化促进空间重新定向和有效的杀戮。相反,TPP途径的上游输入定义了调节策略,具有新的周质调节剂RTK,显示出与S.Marcescens的PPKA激酶相互作用。我们提出了一种模型,由此TPP途径和TAGF的相反动作在射击之后对T6SS重新组装施加延迟,为T6SS的空间重新定向提供机会,以最大化竞争对手靶向的效率。我们的调查结果可以更好地了解细菌细胞如何有效地部署竞争性武器,这对不同多种多发性群落的结构和动态有影响。

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