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Zika 病毒蛋白酶:抗病毒药物靶点。

Zika Virus Protease: An Antiviral Drug Target.

机构信息

Experimental Therapeutics Centre, Agency for Science, Technology and Research (A*STAR), 31 Biopolis way, Nanos, #03-01, 138669, Singapore.

Lee Kong Chian School of Medicine, Nanyang Technological University, EMB 03-07, 59 Nanyang Drive, 636921, Singapore; NTU Institute of Structural Biology, Nanyang Technological University, EMB 06-01, 59 Nanyang Drive, 636921, Singapore.

出版信息

Trends Microbiol. 2017 Oct;25(10):797-808. doi: 10.1016/j.tim.2017.07.001. Epub 2017 Aug 5.

Abstract

The recent outbreak of Zika virus (ZIKV) infection has caused global concern due to its link to severe damage to the brain development of foetuses and neuronal complications in adult patients. A worldwide research effort has been undertaken to identify effective and safe treatment and vaccination options. Among the proposed viral and host components, the viral NS2B-NS3 protease represents an attractive drug target due to its essential role in the virus life cycle. Here, we outline recent progress in studies on the Zika protease. Biochemical, biophysical, and structural studies on different protease constructs provide new insight into the structure and activity of the protease. The unlinked construct displays higher enzymatic activity and better mimics the native state of the enzyme and therefore is better suited for drug discovery. Furthermore, the structure of the free enzyme adopts a closed conformation and a preformed active site. The availability of a lead fragment hit and peptide inhibitors, as well as the attainability of soakable crystals, suggest that the unlinked construct is a promising tool for drug discovery.

摘要

近期爆发的 Zika 病毒(ZIKV)感染引起了全球关注,因为它与胎儿大脑发育严重受损以及成年患者的神经并发症有关。全球范围内都在努力寻找有效和安全的治疗和疫苗接种选择。在提出的病毒和宿主成分中,病毒 NS2B-NS3 蛋白酶由于在病毒生命周期中的重要作用,成为一个有吸引力的药物靶点。在这里,我们概述了 Zika 蛋白酶研究的最新进展。对不同蛋白酶结构的生化、生物物理和结构研究为蛋白酶的结构和活性提供了新的认识。无连接结构显示出更高的酶活性,更好地模拟了酶的天然状态,因此更适合药物发现。此外,游离酶的结构采用封闭构象和预先形成的活性位点。先导片段命中和肽抑制剂的可用性,以及可浸泡晶体的获得,表明无连接结构是药物发现的有前途的工具。

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