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真核生物翻译起始因子4G(eIF4G)-真核生物翻译起始因子4E(eIF4E)复合物是鼻病毒2A蛋白酶直接切割的靶标。

The eIF4G-eIF4E complex is the target for direct cleavage by the rhinovirus 2A proteinase.

作者信息

Haghighat A, Svitkin Y, Novoa I, Kuechler E, Skern T, Sonenberg N

机构信息

Department of Biochemistry, Faculty of Medicine, McGill University, Montréal, Quebec, Canada.

出版信息

J Virol. 1996 Dec;70(12):8444-50. doi: 10.1128/JVI.70.12.8444-8450.1996.

Abstract

The 2A proteinases (2Apro) of certain picornaviruses induce the cleavage of the eIF4G subunit of the cap-binding protein complex, eIF4F. Several reports have demonstrated that 2Apro of rhinovirus and coxsackievirus B4 cleave eIF4G directly. However, it was suggested that in poliovirus infection, the 2Apro induces the activation of a cellular proteinase which in turn cleaves eIF4G. Furthermore, it is not clear whether eIF4G is cleaved as part of the eIF4F complex or as an individual polypeptide. To address these issues, recombinant eIF4G was purified from Sf9 insect cells and tested for cleavage by purified rhinovirus 2Apro. Here we report that eIF4G alone is a relatively poor substrate for cleavage by the rhinovirus 2Apro. However, an eIF4G-eIF4E complex is cleaved efficiently by the 2Apro, suggesting that eIF4F is a preferred substrate for cleavage by rhinovirus 2Apro. Furthermore, 2Apr drastically reduced the translation of a capped mRNA. An eIF4G-eIF4E complex, but not eIF4G alone, was required to restore translation.

摘要

某些微小核糖核酸病毒的2A蛋白酶(2Apro)可诱导帽结合蛋白复合物eIF4F的eIF4G亚基发生裂解。多项报告表明,鼻病毒和柯萨奇病毒B4的2Apro可直接裂解eIF4G。然而,有人提出在脊髓灰质炎病毒感染过程中,2Apro会诱导一种细胞蛋白酶的激活,进而裂解eIF4G。此外,目前尚不清楚eIF4G是作为eIF4F复合物的一部分被裂解,还是作为单个多肽被裂解。为了解决这些问题,从Sf9昆虫细胞中纯化了重组eIF4G,并检测其被纯化的鼻病毒2Apro裂解的情况。在此我们报告,单独的eIF4G是鼻病毒2Apro相对较差的裂解底物。然而,eIF4G - eIF4E复合物可被2Apro有效裂解,这表明eIF4F是鼻病毒2Apro裂解的首选底物。此外,2Apro显著降低了带帽mRNA的翻译。恢复翻译需要eIF4G - eIF4E复合物,而不是单独的eIF4G。

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