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Biophysical Mechanism of Protein Export by Bacterial Type III Secretion System

机译:细菌III分泌系统蛋白质出口的生物物理机制

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Type III secretion system (T3SS) is a protein injection nano-machine consisting of syringe and needle like structure spanning bacterial inner and outer membranes. Bacteria insert the tip of T3SS needle to host cell membranes, and deliver effector proteins directly into host cells via T3SS to prime the host cell environment for infection. Thus inhibition of T3SS would be a potent strategy for suppressing bacterial infection. We previously demonstrated that T3SS needle rotates by proton-motive force (PMF) with the same mechanism as two evolutionally related rotary protein motors, flagellum and ATP synthase (FASEB J., 27, 2013, Ohgita et al.). Inhibition of needle rotation resulted in suppression of effector secretion, indicating the requirement of needle rotation for effector export. Simulation analysis of protein export by the T3SS needle suggests the importance of a hydrophobic helical groove formed by the conserved aromatic residue in the needle components. Based on these results, we have proposed a novel model of protein export by the T3SS needle, in which effector proteins are exported by PMF-dependent needle rotation oppositely to the hydrophobic helical groove in the needle. Quantitative examinations of the correlation between the speeds of T3SS rotation and the amount of effector export support this model. In this review, we summarize our current understanding of T3SS, and discuss our novel model of the protein export mechanism of T3SS based on the needle rotation.
机译:III型分泌系统(T3SS)是一种蛋白质注射纳米机,包括注射器和针状结构跨细菌内膜和外膜。细菌将T3SS针的尖端插入宿主细胞膜,并通过T3SS将效应蛋白直接进入宿主细胞中以使宿主细胞环境进行感染。因此,T3S的抑制将是抑制细菌感染的有效策略。我们之前证明T3SS针通过质子 - 动力(PMF)旋转,具有与两个进化相关的旋转蛋白质电动机,鞭毛和ATP合酶(Faseb J.,2013,Ohgita等人)相同的机制。针旋转的抑制导致抑制效应分泌,表明针对效应输出的针头旋转的要求。 T3SS针的蛋白质导出模拟分析表明,通过针部件中保守的芳族残留物形成的疏水螺旋槽的重要性。基于这些结果,我们提出了T3SS针的新型蛋白质导出模型,其中效应蛋白通过与针中的疏水螺旋槽相对的PMF依赖的针头旋转出口。 T3SS旋转速度与效应器出口量之间的相关性的定量检查和效应输出量支持该模型。在这篇综述中,我们总结了我们目前对T3S的理解,并根据针头旋转讨论T3SS蛋白质出口机制的新模型。

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