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pKID通过具有非天然相互作用的无结构过渡态与KIX结合。

pKID Binds to KIX via an Unstructured Transition State with Nonnative Interactions.

作者信息

Dahal Liza, Kwan Tristan O C, Shammas Sarah L, Clarke Jane

机构信息

Department of Chemistry, University of Cambridge, Cambridge, United Kingdom.

Department of Chemistry, University of Cambridge, Cambridge, United Kingdom.

出版信息

Biophys J. 2017 Dec 19;113(12):2713-2722. doi: 10.1016/j.bpj.2017.10.016.

Abstract

Understanding the detailed mechanism of interaction of intrinsically disordered proteins with their partners is crucial to comprehend their functions in signaling and transcription. Through its interaction with KIX, the disordered pKID region of CREB protein is central in the transcription of cAMP responsive genes, including those involved in long-term memory. Numerous simulation studies have investigated these interactions. Combined with experimental results, these can provide valuable and comprehensive understanding of the mechanisms involved. Here, we probe the transition state of this interaction experimentally through analyzing the kinetic effect of mutating both interface and solvent exposed residues in pKID. We show that very few specific interactions between pKID and KIX are required in the initial binding process. Only a small number of weak interactions are formed at the transition state, including nonnative interactions, and most of the folding occurs after the initial binding event. These properties are consistent with computational results and also the majority of experimental studies of intrinsically disordered protein coupled folding and binding in other protein systems, suggesting that these may be common features.

摘要

了解内在无序蛋白质与其伴侣相互作用的详细机制对于理解它们在信号传导和转录中的功能至关重要。通过与KIX相互作用,CREB蛋白的无序pKID区域在cAMP反应基因的转录中起核心作用,这些基因包括参与长期记忆的基因。许多模拟研究已经对这些相互作用进行了调查。结合实验结果,这些研究可以提供对所涉及机制的有价值且全面的理解。在这里,我们通过分析pKID中界面和溶剂暴露残基突变的动力学效应,对这种相互作用的过渡态进行实验探究。我们表明,在初始结合过程中,pKID与KIX之间只需要很少的特异性相互作用。在过渡态仅形成少量弱相互作用,包括非天然相互作用,并且大多数折叠发生在初始结合事件之后。这些特性与计算结果以及其他蛋白质系统中内在无序蛋白质耦合折叠和结合的大多数实验研究一致,表明这些可能是共同特征。

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