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脊髓灰质炎病毒VP0成熟切割的催化作用不是由VP2的丝氨酸10介导的。

Catalysis of poliovirus VP0 maturation cleavage is not mediated by serine 10 of VP2.

作者信息

Harber J J, Bradley J, Anderson C W, Wimmer E

机构信息

Department of Microbiology, State University of New York, Stony Brook 11794.

出版信息

J Virol. 1991 Jan;65(1):326-34. doi: 10.1128/JVI.65.1.326-334.1991.

Abstract

The maturation of the poliovirus capsid occurs as the result of a single unexplained proteolytic event during which 58 to 59 copies of the 60 VP0 capsid protein precursors are cleaved. An autocatalytic mechanism for cleavage of VP0 to VP4 and VP2 was proposed by Arnold et al. (E. Arnold, M. Luo, G. Vriend, M. G. Rossman, A. C. Palmenberg, G. D. Parks, M. J. Nicklin, and E. Wimmer, Proc. Natl. Acad. Sci. USA 84:21-25, 1987) in which serine 10 of VP2 is activated by virion RNA to catalyze VP4-VP2 processing. The hypothesis rests on the observation that a hydrogen bond was observed between serine 10 of VP2 (S2010) and the carboxyl terminus of VP4 in three mature picornaviral atomic structures: rhinovirus 14, mengovirus, and poliovirus type 1 (Mahoney). We constructed mutant viruses with cysteine (S2010C) or alanine (S2010A) replacing serine 10 of VP2; these exhibited normal proteolytic processing of VP0. While our results do not exclude an autocatalytic mechanism for the maturation cleavage, they do eliminate the conserved S2010 residue as the catalytic amino acid.

摘要

脊髓灰质炎病毒衣壳的成熟是由一次原因不明的蛋白水解事件导致的,在此过程中,60个VP0衣壳蛋白前体中的58至59个拷贝被切割。Arnold等人(E. Arnold、M. Luo、G. Vriend、M. G. Rossman、A. C. Palmenberg、G. D. Parks、M. J. Nicklin和E. Wimmer,《美国国家科学院院刊》84:21 - 25,1987年)提出了一种VP0切割为VP4和VP2的自催化机制,其中VP2的丝氨酸10被病毒粒子RNA激活,以催化VP4 - VP2的加工过程。该假说基于以下观察结果:在三种成熟的小核糖核酸病毒原子结构(鼻病毒14、脑心肌炎病毒和脊髓灰质炎病毒1型(Mahoney株))中,观察到VP2的丝氨酸10(S2010)与VP4的羧基末端之间存在氢键。我们构建了用半胱氨酸(S2010C)或丙氨酸(S2010A)取代VP2丝氨酸10的突变病毒;这些病毒表现出VP0正常的蛋白水解加工过程。虽然我们的结果不排除成熟切割存在自催化机制,但它们确实排除了保守的S2010残基作为催化氨基酸的可能性。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/e4a3/240521/7449a4c0441c/jvirol00044-0350-a.jpg

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