Infection Biology, Biozentrum der Universität Basel, Basel, Switzerland.
EMBO J. 2010 Jun 2;29(11):1928-40. doi: 10.1038/emboj.2010.84. Epub 2010 May 7.
The assembly of the Yersinia enterocolitica type III secretion injectisome was investigated by grafting fluorescent proteins onto several components, YscC (outer-membrane (OM) ring), YscD (forms the inner-membrane (IM) ring together with YscJ), YscN (ATPase), and YscQ (putative C ring). The recombinant injectisomes were functional and appeared as fluorescent spots at the cell periphery. Epistasis experiments with the hybrid alleles in an array of injectisome mutants revealed a novel outside-in assembly order: whereas YscC formed spots in the absence of any other structural protein, formation of YscD foci required YscC, but not YscJ. We therefore propose that the assembly starts with YscC and proceeds through the connector YscD to YscJ, which was further corroborated by co-immunoprecipitation experiments. Completion of the membrane rings allowed the subsequent assembly of cytosolic components. YscN and YscQ attached synchronously, requiring each other, the interacting proteins YscK and YscL, but no further injectisome component for their assembly. These results show that assembly is initiated by the formation of the OM ring and progresses inwards to the IM ring and, finally, to a large cytosolic complex.
肠侵袭性大肠杆菌 III 型分泌系统注射器的组装通过将荧光蛋白嫁接到几个组件上进行了研究,这些组件包括 YscC(外膜(OM)环)、YscD(与 YscJ 一起形成内膜(IM)环)、YscN(ATP 酶)和 YscQ(假定的 C 环)。重组注射器是功能性的,在细胞边缘呈现为荧光斑点。在一系列注射器突变体的杂种等位基因的上位性实验中,揭示了一种新的从外向内的组装顺序:尽管 YscC 在没有任何其他结构蛋白的情况下形成斑点,但 YscD 焦点的形成需要 YscC,但不需要 YscJ。因此,我们提出组装从 YscC 开始,通过连接器 YscD 进行到 YscJ,这进一步通过共免疫沉淀实验得到证实。膜环的完成允许随后组装细胞质成分。YscN 和 YscQ 同步附着,彼此需要,相互作用的蛋白质 YscK 和 YscL,但不需要其他注射器组件进行组装。这些结果表明,组装是由 OM 环的形成引发的,并向内进行到 IM 环,最后形成一个大的细胞质复合物。
