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肠道病毒 71 型 2A 蛋白酶的构象可塑性。

Conformational plasticity of the 2A proteinase from enterovirus 71.

机构信息

State Key Laboratory of Cellular Stress Biology, School of Life Sciences, Xiamen University, Xiamen, China.

出版信息

J Virol. 2013 Jul;87(13):7348-56. doi: 10.1128/JVI.03541-12. Epub 2013 Apr 24.

Abstract

The 2A proteinase (2A(pro)) is an enterovirally encoded cysteine protease that plays essential roles in both the processing of viral precursor polyprotein and the hijacking of host cell translation and other processes in the virus life cycle. Crystallographic studies of 2A(pro) from enterovirus 71 (EV71) and its interaction with the substrate are reported here. EV71 2A(pro) was comprised of an N-terminal domain of a four-stranded antiparallel β sheet and a C-terminal domain of a six-stranded antiparallel β barrel with a tightly bound zinc atom. Unlike in other 2A(pro) structures, there is an open cleft across the surface of the protein in an open conformation. As demonstrated by the crystallographic studies and modeling of the complex structure, the open cleft could be fitted with the substrate. On comparison 2A(pro) of EV71 to those of the human rhinovirus 2 and coxsackievirus B4, the open conformation could be closed with a hinge motion in the bII2 and cII β strands. This was supported by molecular dynamic simulation. The structural variation among different 2A(pro) structures indicates a conformational flexibility in the substrate-binding cleft. The open structure provides an accessible framework for the design and development of therapeutics against the viral target.

摘要

2A 蛋白水解酶(2A(pro)) 是一种肠道病毒编码的半胱氨酸蛋白酶,在病毒生命周期中,它在病毒前体多蛋白的加工以及劫持宿主细胞翻译和其他过程中都发挥着重要作用。本文报道了肠道病毒 71(EV71)的 2A(pro)及其与底物相互作用的晶体学研究。EV71 2A(pro)由一个四股反平行β 片层的 N 端结构域和一个六股反平行β 桶的 C 端结构域组成,其中紧密结合一个锌原子。与其他 2A(pro) 结构不同,在开放构象中,蛋白质表面有一个开放的裂隙。晶体学研究和复合物结构建模表明,开放裂隙可以容纳底物。通过将 EV71 的 2A(pro)与人类鼻病毒 2 和柯萨奇病毒 B4 的 2A(pro)进行比较,发现 bII2 和 cIIβ 链的铰链运动可以使开放构象闭合。这一结论得到了分子动力学模拟的支持。不同 2A(pro) 结构之间的结构差异表明其在底物结合裂隙中具有构象灵活性。开放结构为针对病毒靶标设计和开发治疗药物提供了一个可及的框架。

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