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人VCP/p97的D1-D2连接体在D1结构域的不对称性和ATP酶活性中的作用

Role of the D1-D2 Linker of Human VCP/p97 in the Asymmetry and ATPase Activity of the D1-domain.

作者信息

Tang Wai Kwan, Xia Di

机构信息

Laboratory of Cell Biology, Center for Cancer Research, National Cancer Institute, National Institutes of Health, Bethesda, MD 20892, USA.

出版信息

Sci Rep. 2016 Jan 28;6:20037. doi: 10.1038/srep20037.

Abstract

Human AAA(+) protein p97 consists of an N-domain and two tandem ATPase domains D1 and D2, which are connected by the N-D1 and the D1-D2 linkers. Inclusion of the D1-D2 linker, a 22-amino acid peptide, at the end of p97 N-D1 truncate has been shown to activate ATP hydrolysis of its D1-domain, although the mechanism of activation remains unclear. Here, we identify the N-terminal half of this linker, highly conserved from human to fungi, is essential for the ATPase activation. By analyzing available crystal structures, we observed that the D1-D2 linker is capable of inducing asymmetry in subunit association into a p97 hexamer. This observation is reinforced by two new crystal structures, determined in the present work. The effect of D1-D2 linker on the ATPase activity of the D1-domain is correlated to the side-chain conformation of residue R359, a trans-acting arginine-finger residue essential for ATP hydrolysis of the D1-domain. The activation in D1-domain ATPase activity by breaking perfect six-fold symmetry implies functional importance of asymmetric association of p97 subunits, the extent of which can be determined quantitatively by the metric Asymmetric Index.

摘要

人类AAA(+)蛋白p97由一个N结构域和两个串联的ATP酶结构域D1和D2组成,它们通过N-D1和D1-D2连接子相连。在p97 N-D1截短体的末端包含一个22个氨基酸的肽段D1-D2连接子,已被证明可激活其D1结构域的ATP水解,尽管激活机制尚不清楚。在这里,我们发现该连接子的N端一半从人类到真菌高度保守,对ATP酶激活至关重要。通过分析现有的晶体结构,我们观察到D1-D2连接子能够诱导亚基缔合形成p97六聚体时的不对称性。本研究中确定的两个新晶体结构进一步证实了这一观察结果。D1-D2连接子对D1结构域ATP酶活性的影响与残基R359的侧链构象相关,R359是D1结构域ATP水解所必需的反式作用精氨酸指残基。通过打破完美的六重对称性来激活D1结构域的ATP酶活性,意味着p97亚基不对称缔合具有功能重要性,其程度可以通过不对称指数来定量确定。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/7614/4730245/2e33c08f8a85/srep20037-f1.jpg

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