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Identification of Atg3 as an intrinsically disordered polypeptide yields insights into the molecular dynamics of autophagy-related proteins in yeast

机译:将Atg3鉴定为内在无序的多肽可深入了解酵母中自噬相关蛋白的分子动力学

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摘要

The mechanism of autophagy relies on complex cell signaling and regulatory processes. Each cell contains many proteins that lack a rigid 3-dimensional structure under physiological conditions. These dynamic proteins, called intrinsically disordered proteins (IDPs) and protein regions (IDPRs), are predominantly involved in cell signaling and regulation. Yet, very little is known about their presence among proteins of the core autophagy machinery. In this work, we characterized the autophagy protein Atg3 from yeast and human along with 2 variants to show that Atg3 is an IDPRs-containing protein and that disorder/order predicted for these proteins from their amino acid sequence corresponds to their experimental characteristics. Based on this consensus, we applied the same prediction methods to all known Atg proteins from Saccharomyces cerevisiae. The data presented here provide an insight into the structural dynamics of each Atg protein. They also show that intrinsic disorder at various levels has to be taken into consideration for about half of the Atg proteins. This work should become a useful tool that will facilitate and encourage exploration of protein intrinsic disorder in autophagy.
机译:自噬的机制依赖于复杂的细胞信号传导和调节过程。每个细胞包含许多在生理条件下缺乏刚性3维结构的蛋白质。这些动态蛋白质称为内在无序蛋白质(IDP)和蛋白质区域(IDPR),主要参与细胞信号传导和调控。然而,关于它们在核心自噬机制蛋白中的存在知之甚少。在这项工作中,我们表征了来自酵母和人类的自噬蛋白Atg3以及2个变体,以显示Atg3是一种含IDPRs的蛋白,从这些蛋白的氨基酸序列预测的这些蛋白的失序/顺序与其实验特征相对应。基于此共识,我们将相同的预测方法应用于酿酒酵母中所有已知的Atg蛋白。此处提供的数据可洞悉每种Atg蛋白的结构动力学。他们还表明,对于大约一半的Atg蛋白,必须考虑各种水平的内在疾病。这项工作应成为一个有用的工具,将促进和鼓励自噬中蛋白质内在疾病的探索。

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