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非洲猪瘟病毒 pS273R 蛋白酶的晶体结构及其抑制剂设计的意义。

Crystal Structure of African Swine Fever Virus pS273R Protease and Implications for Inhibitor Design.

机构信息

State Key Laboratory of Medicinal Chemical Biology and College of Pharmacy, Nankai University, Tianjin, People's Republic of China.

Drug Discovery Center for Infectious Diseases, Nankai University, Tianjin, People's Republic of China.

出版信息

J Virol. 2020 May 4;94(10). doi: 10.1128/JVI.02125-19.

Abstract

African swine fever (ASF) is a highly contagious hemorrhagic viral disease of domestic and wild pigs that is responsible for serious economic and production losses. It is caused by the African swine fever virus (ASFV), a large and complex icosahedral DNA virus of the family. Currently, there is no effective treatment or approved vaccine against the ASFV. pS273R, a specific SUMO-1 cysteine protease, catalyzes the maturation of the pp220 and pp62 polyprotein precursors into core-shell proteins. Here, we present the crystal structure of the ASFV pS273R protease at a resolution of 2.3 Å. The overall structure of the pS273R protease is represented by two domains named the "core domain" and the N-terminal "arm domain." The "arm domain" contains the residues from M1 to N83, and the "core domain" contains the residues from N84 to A273. A structure analysis reveals that the "core domain" shares a high degree of structural similarity with chlamydial deubiquitinating enzyme, sentrin-specific protease, and adenovirus protease, while the "arm domain" is unique to ASFV. Further, experiments indicated that the "arm domain" plays an important role in maintaining the enzyme activity of ASFV pS273R. Moreover, based on the structural information of pS273R, we designed and synthesized several peptidomimetic aldehyde compounds at a submolar 50% inhibitory concentration, which paves the way for the design of inhibitors to target this severe pathogen. African swine fever virus, a large and complex icosahedral DNA virus, causes a deadly infection in domestic pigs. In addition to Africa and Europe, countries in Asia, including China, Vietnam, and Mongolia, were negatively affected by the hazards posed by ASFV outbreaks in 2018 and 2019, at which time more than 30 million pigs were culled. Until now, there has been no vaccine for protection against ASFV infection or effective treatments to cure ASF. Here, we solved the high-resolution crystal structure of the ASFV pS273R protease. The pS273R protease has a two-domain structure that distinguishes it from other members of the SUMO protease family, while the unique "arm domain" has been proven to be essential for its hydrolytic activity. Moreover, the peptidomimetic aldehyde compounds designed to target the substrate binding pocket exert prominent inhibitory effects and can thus be used in a potential lead for anti-ASFV drug development.

摘要

非洲猪瘟(ASF)是一种高度传染性的出血性病毒性疾病,可导致家猪和野猪严重的经济和生产损失。它是由非洲猪瘟病毒(ASFV)引起的,ASFV 是一种大型复杂的二十面体 DNA 病毒,属于 科。目前,尚无针对 ASFV 的有效治疗方法或批准的疫苗。pS273R 是一种特定的 SUMO-1 半胱氨酸蛋白酶,可催化 pp220 和 pp62 多蛋白前体成熟为核壳蛋白。在这里,我们展示了分辨率为 2.3 Å 的 ASFV pS273R 蛋白酶的晶体结构。pS273R 蛋白酶的整体结构由两个结构域表示,分别称为“核心结构域”和 N 端“臂结构域”。“臂结构域”包含 M1 到 N83 的残基,“核心结构域”包含 N84 到 A273 的残基。结构分析表明,“核心结构域”与衣原体去泛素化酶、 特有的蛋白酶和腺病毒蛋白酶具有高度的结构相似性,而“臂结构域”则是 ASFV 所特有的。此外,实验表明,“臂结构域”在维持 ASFV pS273R 的酶活性方面起着重要作用。此外,基于 pS273R 的结构信息,我们设计并合成了几种亚摩尔 50%抑制浓度的肽模拟醛化合物,为针对这种严重病原体的抑制剂设计铺平了道路。非洲猪瘟病毒是一种大型复杂的二十面体 DNA 病毒,会在家猪中引起致命感染。除了非洲和欧洲,亚洲的一些国家,包括中国、越南和蒙古,在 2018 年和 2019 年也受到了 ASF 爆发带来的危害的负面影响,当时有超过 3000 万头猪被扑杀。到目前为止,还没有针对 ASFV 感染的疫苗或治疗 ASF 的有效方法。在这里,我们解决了 ASFV pS273R 蛋白酶的高分辨率晶体结构。pS273R 蛋白酶具有二结构域结构,与其他 SUMO 蛋白酶家族成员区分开来,而独特的“臂结构域”已被证明对其水解活性至关重要。此外,设计用于靶向底物结合口袋的肽模拟醛化合物具有显著的抑制作用,因此可作为抗 ASFV 药物开发的潜在先导化合物。

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