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猿猴病毒40蛋白在无细胞系统中的磷酸化作用。

Phosphorylation of simian virus 40 proteins in a cell-free system.

作者信息

Tan K B, Sokol F

出版信息

J Virol. 1973 Oct;12(4):696-703. doi: 10.1128/JVI.12.4.696-703.1973.

Abstract

We have shown previously that all the structural proteins of simian virus 40 (SV40) are phosphoproteins. Virus phosphorylated in vivo could be further phosphorylated with exogenous cellular protein kinases in a cell-free system containing gamma-(32)P-ATP as phosphate donor. In intact infectious virus only polypeptides 1 and 2 (mol wt 49,000 and 40,800, respectively) were further phosphorylated in vitro. However, when infectious SV40 was partially disrupted, treated with nucleases, and then phosphorylated in vitro, all five structural polypeptides accepted additional phosphate groups. Similarly, all polypeptides of intact empty capsids, derived from infected cells, were further phosphorylated in vitro. Phosphorylation of empty capsids and infectious SV40 in vitro was enhanced from 4- to 11-fold after prior treatment of virus with alkali. The phosphate group was linked only to serine residues of the viral polypeptides phosphorylated both in vitro and in vivo.

摘要

我们之前已经表明,猿猴病毒40(SV40)的所有结构蛋白都是磷蛋白。在含有γ-(32)P-ATP作为磷酸盐供体的无细胞系统中,体内磷酸化的病毒可以被外源细胞蛋白激酶进一步磷酸化。在完整的感染性病毒中,只有多肽1和2(分子量分别为49,000和40,800)在体外被进一步磷酸化。然而,当感染性SV40被部分破坏、用核酸酶处理,然后在体外磷酸化时,所有五种结构多肽都接受了额外的磷酸基团。同样,来自感染细胞的完整空衣壳的所有多肽在体外也被进一步磷酸化。在用碱预先处理病毒后,空衣壳和感染性SV40在体外的磷酸化增强了4至11倍。磷酸基团仅与在体外和体内都被磷酸化的病毒多肽的丝氨酸残基相连。

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