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Combination of Two Separate Binding Domains Defines Stoichiometry between Type III Secretion System Chaperone IpgC and Translocator Protein IpaB

机译:两个单独的结合域的组合定义了III型分泌系统伴侣IpgC和易位蛋白IpaB之间的化学计量

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摘要

Type III secretion systems (TTSSs) utilized by enteropathogenic bacteria require the presence of small, acidic virulence-associated chaperones for effective host cell infection. We adopted a combination of biochemical and cellular techniques to define the chaperone binding domains (CBDs) in the translocators IpaB and IpaC associated with the chaperone IpgC from Shigella flexneri. We identified a novel CBD in IpaB and furthermore precisely mapped the boundaries of the CBDs in both translocator proteins. In IpaC a single binding domain associates with IpgC. In IpaB, we show that the binding of the newly characterized CBD is essential in maintaining the ternary arrangement of chaperone-translocator complex. This hitherto unknown function is reflected in the co-crystal structure as well, with an IpgC dimer bound to an IpaB fragment comprising both CBDs. Moreover, in the absence of this novel CBD the IpaB/IpgC complex aggregates. This dual-recognition of a domain in the protein by the chaperone in facilitating the correct chaperone-substrate organization describes a new function for the TTSS associated chaperone-substrate complexes.
机译:肠致病细菌利用的III型分泌系统(TTSS)需要存在与酸性毒力相关的小分子伴侣,才能有效感染宿主细胞。我们采用了生化和细胞技术的组合,以在易位志贺氏菌伴侣蛋白IpgC相关的易位蛋白IpaB和​​IpaC中定义伴侣蛋白结合域(CBD)。我们在IpaB中鉴定了一种新型的CBD,并在两个易位蛋白中精确定位了CBD的边界。在IpaC中,单个绑定域与IpgC相关联。在IpaB中,我们表明,新近表征的CBD的结合对于维持分子伴侣-转运子复合体的三元排列至关重要。迄今未知的功能也反映在共晶体结构中,IpgC二聚体与包含两个CBD的IpaB片段结合。此外,在缺乏这种新颖的CBD的情况下,IpaB / IpgC复合物会聚集。分子伴侣对蛋白质中结构域的双重识别有助于正确的分子伴侣-底物组织,它为TTSS相关的分子伴侣-底物复合物提供了新功能。

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