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Structural Basis for Ubiquitin Recognition by a Novel Domain from Human Phospholipase A2-activating Protein*

机译:从人磷脂酶A2激活蛋白的新域识别泛素的结构基础*

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摘要

Ubiquitin (Ub) is an essential modifier conserved in all eukaryotes from yeast to human. Phospholipase A2-activating protein (PLAA), a mammalian homolog of yeast DOA1/UFD3, has been proposed to be able to bind with Ub, which plays important roles in endoplasmic reticulum-associated degradation, vesicle formation, and DNA damage response. We have identified a core domain from the PLAA family ubiquitin-binding region of human PLAA (residues 386–465, namely PFUC) that can bind Ub and elucidated its solution structure and Ub-binding mode by NMR approaches. The PFUC domain possesses equal population of two conformers in solution by cis/trans-isomerization, whereas the two isomers exhibit almost equivalent Ub binding abilities. This domain structure takes a novel fold consisting of four β-strands and two α-helices, and the Ub-binding site on PFUC locates in the surface of α2-helix, which is to some extent analogous to those of UBA, CUE, and UIM domains. This study provides structural basis and biochemical information for Ub recognition of the novel PFU domain from a PLAA family protein that may connect ubiquitination and degradation in endoplasmic reticulum-associated degradation.
机译:泛素(Ubquitin)(Ub)是从酵母到人的所有真核生物中保守的必需修饰剂。有人提出磷脂酶A2激活蛋白(PLAA)是酵母DOA1 / UFD3的哺乳动物同源物,能够与Ub结合,Ub在与内质网相关的降解,囊泡形成和DNA损伤反应中起重要作用。我们从人PLAA的PLAA家族泛素结合区(残基386–465,即PFUC)中确定了一个核心域,可以结合Ub,并通过NMR方法阐明了其溶液结构和Ub结合模式。通过顺式/反式异构化,PFUC结构域在溶液中具有相等的两个构象体群体,而两个异构体表现出几乎相等的Ub结合能力。该结构域结构具有新颖的折叠结构,由四个β链和两个α螺旋组成,并且PFUC上的Ub结合位点位于α2-螺旋的表面,在某种程度上类似于UBA,CUE和UIM域。这项研究为Ub识别来自PLAA家族蛋白的新型PFU结构域提供了结构基础和生化信息,该蛋白可能与内质网相关降解中的泛素化和降解有关。

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