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自噬E2酶Atg10的结构

Structure of the autophagic E2 enzyme Atg10.

作者信息

Hong Seung Beom, Kim Byeong-Won, Kim Jun Hoe, Song Hyun Kyu

机构信息

School of Life Sciences and Biotechnology, Korea University, Seoul 136-701, Republic of Korea.

出版信息

Acta Crystallogr D Biol Crystallogr. 2012 Oct;68(Pt 10):1409-17. doi: 10.1107/S0907444912034166. Epub 2012 Sep 18.

Abstract

Autophagy is a regulated degradation pathway that plays a critical role in all eukaryotic life cycles. One interesting feature of the core autophagic process, autophagosome formation, is similar to ubiquitination. One of two autophagic E2 enzymes, Atg10, interacts with Atg7 to receive Atg12, a ubiquitin-like molecule, and is also involved in the Atg12-Atg5 conjugation reaction. To date, no information on the interaction between Atg10 and Atg7 has been reported, although structural information is available pertaining to the individual components. Here, the crystal structure of Atg10 from Saccharomyces cerevisiae is described at 2.7 Å resolution. A significant improvement of the diffraction limit by heavy-atom derivatization was essential for structure determination. The core fold of yeast Atg10 is well conserved compared with those of Atg3 and other E2 enzymes. In contrast to other E2 enzymes, however, the autophagic E2 enzymes Atg3 and Atg10 possess insertion regions in the middle of the core fold and may be involved in protein function. The missing segment, which was termed the `FR-region', in Atg10 may be important for interaction with the E1 enzyme Atg7. This study provides a framework for understanding the E2 conjugation reaction in autophagy.

摘要

自噬是一种受调控的降解途径,在所有真核生物生命周期中发挥关键作用。核心自噬过程(自噬体形成)的一个有趣特征与泛素化相似。两种自噬E2酶之一的Atg10与Atg7相互作用以接收类泛素分子Atg12,并且还参与Atg12-Atg5缀合反应。尽管已有关于各个组分的结构信息,但迄今为止,尚未有关于Atg10与Atg7之间相互作用的报道。在此,以2.7 Å分辨率描述了来自酿酒酵母的Atg10的晶体结构。通过重原子衍生化显著提高衍射极限对于结构测定至关重要。与Atg3和其他E2酶相比,酵母Atg10的核心折叠结构高度保守。然而,与其他E2酶不同,自噬E2酶Atg3和Atg10在核心折叠结构中间具有插入区域,可能与蛋白质功能有关。Atg10中缺失的片段(称为“FR区域”)可能对于与E1酶Atg7的相互作用很重要。这项研究为理解自噬中的E2缀合反应提供了一个框架。

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