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重组流感病毒聚合酶:核酸内切酶活性对病毒5'和3'末端的需求。

Recombinant influenza virus polymerase: requirement of both 5' and 3' viral ends for endonuclease activity.

作者信息

Hagen M, Chung T D, Butcher J A, Krystal M

机构信息

Department of Virology, Bristol-Myers Squibb Pharmaceutical Research Institute, Princeton, New Jersey 08540.

出版信息

J Virol. 1994 Mar;68(3):1509-15. doi: 10.1128/JVI.68.3.1509-1515.1994.

Abstract

Influenza virus polymerase complexes that were expressed in the absence of genomic viral RNA and nucleoprotein were examined for endonuclease activity and transcriptase ability in vitro. Nuclear extracts of cells that express influenza virus polymerase through recombinant vaccinia virus infection did not display specific endonuclease activity in vitro. This polymerase presumably represents an early form of enzyme present in infected cells prior to ribonucleoprotein assembly. Upon addition of a virus-like model RNA template, containing the partially complementary sequence found at the ends of viral RNA, endonuclease activity is stimulated in a concentration-dependent and sequence-specific manner. Once stimulated, the polymerase is able to elongate from the added viral template. Thus, addition of viral template is required for polymerase activity, while the presence of nucleoprotein is not required for limited transcription. Also, full activation of this recombinant viral polymerase is dependent on the presence of both the 3' and 5' ends of the viral genome, as model RNA containing either end alone could not effectively trigger the endonuclease.

摘要

对在无基因组病毒RNA和核蛋白情况下表达的流感病毒聚合酶复合物进行了体外核酸内切酶活性和转录酶能力检测。通过重组痘苗病毒感染表达流感病毒聚合酶的细胞的核提取物在体外未显示出特异性核酸内切酶活性。这种聚合酶大概代表了在核糖核蛋白组装之前存在于受感染细胞中的早期酶形式。加入含有在病毒RNA末端发现的部分互补序列的病毒样模型RNA模板后,核酸内切酶活性以浓度依赖性和序列特异性方式受到刺激。一旦受到刺激,聚合酶就能够从添加的病毒模板开始延伸。因此,聚合酶活性需要添加病毒模板,而有限转录不需要核蛋白的存在。此外,这种重组病毒聚合酶的完全激活依赖于病毒基因组3'端和5'端的同时存在,因为仅含任何一端的模型RNA都不能有效触发核酸内切酶。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/cfd8/236607/3d440a02de57/jvirol00012-0258-a.jpg

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