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首页> 外文期刊>Journal of Molecular Biology >Mutations in the hydrophobic core of ubiquitin differentially affect its recognition by receptor proteins
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Mutations in the hydrophobic core of ubiquitin differentially affect its recognition by receptor proteins

机译:泛素疏水核心的突变差异性地影响受体蛋白的识别

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摘要

Ubiquitin (Ub) is one of the most highly conserved signaling proteins in eukaryotes. In carrying out its myriad functions, Ub conjugated to substrate proteins interacts with dozens of receptor proteins that link the Ub signal to various biological outcomes. Here we report mutations in conserved residues of Ub's hydrophobic core that have surprisingly potent and specific effects on molecular recognition. Mutant Ubs bind tightly to the Ub-associated domain of the receptor proteins Rad23 and hHR23A but fail to bind the Ub-interacting motif present in the receptors Rpn10 and S5a. Moreover, chains assembled on target substrates with mutant Ubs are unable to support substrate degradation by the proteasome in vitro or sustain viability of yeast cells. The mutations have relatively little effect on Ub's overall structure but reduce its rigidity and cause a slight displacement of the C-terminal beta-sheet, thereby compromising association with Ub-interacting motif but not with Ub-associated domains. These studies emphasize an unexpected role for Ub's core in molecular recognition and suggest that the diversity of protein-protein interactions in which Ub engages placed enormous constraints on its evolvability. (c) 2007 Elsevier Ltd. All rights reserved.
机译:泛素(Ubquitin)(Ub)是真核生物中最保守的信号转导蛋白之一。在执行其多种功能时,与底物蛋白缀合的Ub与数十种受体蛋白相互作用,这些受体蛋白将Ub信号与各种生物学结果相关联。在这里,我们报告了Ub疏水核心保守残基中的突变,这些突变对分子识别具有出乎意料的强大和特殊的作用。突变的Ubs与受体蛋白Rad23和hHR23A的Ub相关域紧密结合,但无法结合受体Rpn10和S5a中存在的Ub相互作用基序。而且,组装在具有突变Ub的靶底物上的链不能支持蛋白酶体在体外对底物的降解或维持酵母细胞的活力。突变对Ub的整体结构影响相对较小,但会降低其刚性,并导致C端β-sheet的轻微移位,从而损害与Ub相互作用的基序的关联,而不损害与Ub相关的域。这些研究强调了Ub核心在分子识别中的出乎意料的作用,并表明Ub参与的蛋白质-蛋白质相互作用的多样性对其可进化性构成了极大的限制。 (c)2007 Elsevier Ltd.保留所有权利。

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