Olsson Jan, Edqvist Petra J, Bröms Jeanette E, Forsberg Ake, Wolf-Watz Hans, Francis Matthew S
Department of Molecular Biology, Umeå University, SE-901 87 Umeå, Sweden.
J Bacteriol. 2004 Jul;186(13):4110-23. doi: 10.1128/JB.186.13.4110-4123.2004.
To establish an infection, Yersinia pseudotuberculosis utilizes a plasmid-encoded type III translocon to microinject several anti-host Yop effectors into the cytosol of target eukaryotic cells. YopD has been implicated in several key steps during Yop effector translocation, including maintenance of yop regulatory control and pore formation in the target cell membrane through which effectors traverse. These functions are mediated, in part, by an interaction with the cognate chaperone, LcrH. To gain insight into the complex molecular mechanisms of YopD function, we performed a systematic mutagenesis study to search for discrete functional domains. We highlighted amino acids beyond the first three N-terminal residues that are dispensable for YopD secretion and confirmed that an interaction between YopD and LcrH is essential for maintenance of yop regulatory control. In addition, discrete domains within YopD that are essential for both pore formation and translocation of Yop effectors were identified. Significantly, other domains were found to be important for effector microinjection but not for pore formation. Therefore, YopD is clearly essential for several discrete steps during efficient Yop effector translocation. Recognition of this modular YopD domain structure provides important insights into the function of YopD.
为了建立感染,假结核耶尔森菌利用一种质粒编码的III型转位装置将几种抗宿主Yop效应蛋白微注射到靶真核细胞的细胞质中。YopD参与了Yop效应蛋白转位过程中的几个关键步骤,包括维持yop调控以及在效应蛋白穿过的靶细胞膜上形成孔道。这些功能部分是通过与同源伴侣蛋白LcrH的相互作用介导的。为了深入了解YopD功能的复杂分子机制,我们进行了一项系统的诱变研究以寻找离散的功能结构域。我们强调了N端前三个残基以外的氨基酸对于YopD分泌是可有可无的,并证实YopD与LcrH之间的相互作用对于维持yop调控至关重要。此外,还鉴定出了YopD中对于Yop效应蛋白的孔道形成和转位都必不可少的离散结构域。值得注意的是,还发现其他结构域对于效应蛋白的微注射很重要,但对于孔道形成不重要。因此,YopD显然对于高效Yop效应蛋白转位过程中的几个离散步骤至关重要。对这种模块化YopD结构域结构的认识为YopD的功能提供了重要的见解。