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仙台病毒C蛋白与L聚合酶蛋白结合以抑制病毒RNA合成。

The Sendai virus C protein binds the L polymerase protein to inhibit viral RNA synthesis.

作者信息

Horikami S M, Hector R E, Smallwood S, Moyer S A

机构信息

Department of Pediatrics, University of Florida, Gainesville, Florida, 32610, USA.

出版信息

Virology. 1997 Sep 1;235(2):261-70. doi: 10.1006/viro.1997.8702.

DOI:10.1006/viro.1997.8702
PMID:9281506
Abstract

The Sendai virus nested set of C proteins which are expressed in an alternative open reading frame from the P mRNA has been shown to downregulate viral RNA synthesis. Utilizing a glutathione S-transferase (gst) C fusion protein (gstC), we have shown that C protein forms a complex with the L, but not the P, subunit of the viral RNA polymerase. When P, L, and gstC are coexpressed, an oligomer of P, through its interaction with L, is also bound to beads. Since binding of C to L in the P-L complex does not disrupt P binding, the C and P binding sites appear to be different. GstC binding to L occurs only when the proteins are coexpressed in the same cell. The gstC, but not gst, protein inhibits viral transcription in vitro, showing that the fusion protein retains biological function. Pulse-chase experiments of the various complexes show that L protein synthesized alone has a half-life of 1. 2 hr, which is increased 12.5-fold by binding P, but is not significantly increased by binding gstC. Analyses of complex formation with truncations of L protein show that the C-terminal 1333 amino acids of L are not required for binding C. The dose-response curves show that replication of the genomic DI-H RNA is more sensitive to inhibition by C protein than is the synthesis of DI leader RNA, suggesting that the downregulation of RNA synthesis may be more complex than just the inhibition of the initiation of RNA synthesis.

摘要

仙台病毒的C蛋白嵌套集在P mRNA的一个替代开放阅读框中表达,已被证明可下调病毒RNA合成。利用谷胱甘肽S-转移酶(gst)C融合蛋白(gstC),我们发现C蛋白与病毒RNA聚合酶的L亚基而非P亚基形成复合物。当P、L和gstC共表达时,P的寡聚体通过与L的相互作用也与珠子结合。由于C在P-L复合物中与L的结合不会破坏P的结合,C和P的结合位点似乎不同。只有当蛋白质在同一细胞中共表达时,gstC才会与L结合。gstC蛋白而非gst蛋白在体外抑制病毒转录,表明融合蛋白保留了生物学功能。对各种复合物的脉冲追踪实验表明,单独合成的L蛋白半衰期为1.2小时,与P结合可使其半衰期增加12.5倍,但与gstC结合则不会显著增加。对L蛋白截短体形成复合物的分析表明,L蛋白的C末端1333个氨基酸对于与C的结合不是必需的。剂量反应曲线表明,基因组DI-H RNA的复制比DI前导RNA的合成对C蛋白的抑制更敏感,这表明RNA合成的下调可能比仅仅抑制RNA合成的起始更为复杂。

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The Sendai virus C protein binds the L polymerase protein to inhibit viral RNA synthesis.仙台病毒C蛋白与L聚合酶蛋白结合以抑制病毒RNA合成。
Virology. 1997 Sep 1;235(2):261-70. doi: 10.1006/viro.1997.8702.
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