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YopN and TyeA Hydrophobic Contacts Required for Regulating Ysc-Yop Type III Secretion Activity by Yersinia pseudotuberculosis

机译:YopN和TyeA疏水性接触物,通过伪结核耶尔森氏菌调节Ysc-Yop III型分泌活性

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摘要

Yersinia bacteria target Yop effector toxins to the interior of host immune cells by the Ysc-Yop type III secretion system. A YopN-TyeA heterodimer is central to controlling Ysc-Yop targeting activity. A + 1 frameshift event in the 3-prime end of yopN can also produce a singular secreted YopN-TyeA polypeptide that retains some regulatory function even though the C-terminal coding sequence of this YopN differs greatly from wild type. Thus, this YopN C-terminal segment was analyzed for its role in type III secretion control. Bacteria producing YopN truncated after residue 278, or with altered sequence between residues 279 and 287, had lost type III secretion control and function. In contrast, YopN variants with manipulated sequence beyond residue 287 maintained full control and function. Scrutiny of the YopN-TyeA complex structure revealed that residue W279 functioned as a likely hydrophobic contact site with TyeA. Indeed, a YopNW279G mutant lost all ability to bind TyeA. The TyeA residue F8 was also critical for reciprocal YopN binding. Thus, we conclude that specific hydrophobic contacts between opposing YopN and TyeA termini establishes a complex needed for regulating Ysc-Yop activity.
机译:耶尔森氏菌通过Ysc-Yop III型分泌系统将Yop效应毒素靶向宿主免疫细胞的内部。 YopN-TyeA异二聚体是控制Ysc-Yop靶向活性的关键。 yopN的3-prime末端的+1移码事件也可以产生单个分泌的YopN-TyeA多肽,即使该YopN的C端编码序列与野生型有很大差异,它仍保留了一些调节功能。因此,分析了该YopN C-末端区段在III型分泌控制中的作用。产生YopN的细菌在残基278之后被截断,或者残基279和287之间的序列发生了改变,失去了III型分泌控制和功能。相反,具有超过残基287的操纵序列的YopN变体保持完全的控制和功能。对YopN-TyeA复合物结构的详细检查显示,残基W279可能是与TyeA的疏水接触位点。实际上,YopNW279G突变体丧失了所有结合TyeA的能力。 TyeA残基F8对相互的YopN结合也至关重要。因此,我们得出结论,相对的YopN和TyeA末端之间的特定疏水接触建立了调节Ysc-Yop活性所需的复合物。

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