State Key Laboratory of Virology, Modern Virology Research Center, College of Life Sciences, Wuhan University, Wuhan, 430072, China.
Virol Sin. 2021 Jun;36(3):438-448. doi: 10.1007/s12250-020-00314-2. Epub 2020 Nov 16.
Human parainfluenza virus type 3 (HPIV3), a member of the Paramyxoviridae family, can cause lower respiratory disease in infants and young children. The phosphoprotein (P) of HPIV3 is an essential cofactor of the viral RNA-dependent RNA polymerase large protein (L). P connects nucleocapsid protein (N) with L to initiate genome transcription and replication. Sumoylation influences many important pathways of the target proteins, and many viral proteins are also themselves sumoylated. In this study, we found that the P of HPIV3 could be sumoylated, and mutation of K492 and K532 to arginine (P) failed to be sumoylated within P, which enhances HPIV3 minigenome activity. Biochemical studies showed that P had no effect on its interactions with N, formation of homo-tetramers and formation of inclusion bodies. Finally, we found that incorporation of K492R/K532R into a recombinant HPIV3 (rHPIV3-P) increased viral production in culture cells, suggesting that sumoylation attenuates functions of P and down-regulates viral replication.
人类副流感病毒 3 型(HPIV3)是副黏病毒科的一员,可导致婴幼儿下呼吸道疾病。HPIV3 的磷蛋白(P)是病毒 RNA 依赖性 RNA 聚合酶大蛋白(L)的必需辅助因子。P 将核衣壳蛋白(N)与 L 连接起来,启动基因组转录和复制。泛素化影响靶蛋白的许多重要途径,许多病毒蛋白本身也被泛素化。在这项研究中,我们发现 HPIV3 的 P 可以被泛素化,并且 K492 和 K532 突变为精氨酸(P)时,P 内的泛素化失败,从而增强了 HPIV3 小基因的活性。生化研究表明,P 对其与 N 的相互作用、同源四聚体的形成和包涵体的形成没有影响。最后,我们发现将 K492R/K532R 掺入重组 HPIV3(rHPIV3-P)中会增加培养细胞中的病毒产量,表明泛素化会削弱 P 的功能并下调病毒复制。
