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The Translocation Domain in Trimeric Autotransporter Adhesins Is Necessary and Sufficient for Trimerization and Autotransportation

机译:三聚体自动转运蛋白粘附素中的易位域对于三聚化和自动转运是必要且充分的

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摘要

Trimeric autotransporter adhesins (TAAs) comprise one of the secretion pathways of the type V secretion system. The mechanism of their translocation across the outer membrane remains unclear, but it most probably occurs by the formation of a hairpin inside the β-barrel translocation unit, leading to transportation of the passenger domain from the C terminus to the N terminus through the lumen of the β-barrel. We further investigated the phenomenon of autotransportation and the rules that govern it. We showed by coexpressing different Escherichia coli immunoglobulin-binding (Eib) proteins that highly similar TAAs could form stochastically mixed structures (heterotrimers). We further investigated this phenomenon by coexpressing two more distantly related TAAs, EibA and YadA. These, however, did not form heterotrimers; indeed, coexpression was lethal to the cells, leading to elimination of one or another of the genes. However, substituting in either protein the barrel of the other one so that the barrels were identical led to formation of heterotrimers as for Eibs. Our work shows that trimerization of the β-barrel, but not the passenger domain, is necessary and sufficient for TAA secretion while the passenger domain is not.
机译:三聚体自转运粘附素(TAA)构成V型分泌系统的分泌途径之一。它们跨外膜易位的机制尚不清楚,但最有可能是通过在β桶易位单元内部形成发夹而导致的,将过客结构域从C末端通过内腔转运到N末端。 β-桶。我们进一步研究了自动运输现象及其控制规则。通过共表达不同的大肠杆菌免疫球蛋白结合(Eib)蛋白,我们发现高度相似的TAA可以形成随机混合的结构(异戊二烯)。我们通过共同表达两个更远相关的TAA,EibA和YadA,进一步研究了这种现象。然而,这些没有形成异源三聚体。实际上,共表达对细胞具有致死性,导致消除了一个或另一个基因。但是,用一种蛋白质取代另一种蛋白质的桶状结构,使该桶状结构相同,会导致形成异源三聚体,就像Eibs一样。我们的工作表明,对β桶进行三聚化,而不对乘客域进行三聚化,对于TAA分泌是必要的,而对于乘客域则不是足够的。

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