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Arrestins: structural disorder creates rich functionality

机译:因素:结构障碍创造丰富的功能

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摘要

Abstract Arrestins are soluble relatively small 44–46 kDa proteins that specifically bind hundreds of active phosphorylated GPCRs and dozens of non-receptor partners. There are binding partners that demonstrate preference for each of the known arrestin conformations: free, receptor-bound, and microtubule-bound. Recent evidence suggests that conformational flexibility in every functional state is the defining characteristic of arrestins. Flexibility, or plasticity, of proteins is often described as structural disorder, in contrast to the fixed conformational order observed in high-resolution crystal structures. However, protein-protein interactions often involve highly flexible elements that can assume many distinct conformations upon binding to different partners. Existing evidence suggests that arrestins are no exception to this rule: their flexibility is necessary for functional versatility. The data on arrestins and many other multi-functional proteins indicate that in many cases, “order” might be artificially imposed by highly non-physiological crystallization conditions and/or crystal packing forces. In contrast, conformational flexibility (and its extreme case, intrinsic disorder) is a more natural state of proteins, representing true biological order that underlies their physiologically relevant functions.
机译:摘要Arcketins是可溶性相对较小的44-46kDa蛋白,其特异性地结合数百个活性磷酸化GPCR和数十种非受体伴侣。有结合伴侣证明了对已知的每个已知的诱导构象的偏好:自由,受体 - 结合和微管状。最近的证据表明,每个功能状态的构象灵活性是逮捕素的定义特征。蛋白质的柔韧性或可塑性通常被描述为结构性障碍,与在高分辨率晶体结构中观察到的固定构象顺序相反。然而,蛋白质 - 蛋白质相互作用通常涉及高度柔性元件,其可以在与不同的合作伙伴结合时呈现许多不同的构象。现有证据表明,逮捕者对此规则没有例外:它们的灵活性是功能多种能力所必需的。 arretins和许多其他多功能蛋白的数据表明,在许多情况下,可以通过高度非生理结晶条件和/或晶体包装力来人工施加“命令”。相比之下,构象灵活性(及其极端情况,内在病症)是更自然的蛋白质状态,代表真正的生物学顺序,使其生理相关的功能归结。

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