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痘苗病毒RNA聚合酶在病毒早期启动子处形成三元复合物:采用非变性凝胶电泳分析

Ternary complex formation by vaccinia virus RNA polymerase at an early viral promoter: analysis by native gel electrophoresis.

作者信息

Hagler J, Shuman S

机构信息

Program in Molecular Biology, Sloan-Kettering Institute, New York, New York 10021.

出版信息

J Virol. 1992 May;66(5):2982-9. doi: 10.1128/JVI.66.5.2982-2989.1992.

Abstract

We have resolved, by native gel electrophoresis, two intermediates in the transcription of a vaccinia virus early gene by the virus-encoded RNA polymerase. Polymerase holoenzyme containing the vaccinia virus early transcription factor (VETF) forms a complex of VETF bound to the promoter as the first step in a pathway leading to establishment of a committed ternary elongation complex. Formation of the VETF-DNA complex is stimulated by magnesium but is uninfluenced by nucleoside triphosphates. A stable binary complex of RNA polymerase bound to DNA is not detected. Assembly of a gel-stable polymerase-DNA complex depends on conditions permissive for RNA synthesis. Nucleotide omission experiments suggest that at least a tetrameric RNA must be made before a ternary complex is stabilized. RNA analysis indicates that complexes containing nascent transcripts 20 nucleotides long are stable and active. Ternary complex formation requires hydrolyzable ATP. This is consistent with an essential role for the ATPase activity of VETF at a step subsequent to DNA binding, as proposed by Broyles (S. S. Broyles, J. Biol. Chem. 266:15545-15548, 1991). The ternary complex, once formed, is resistant to dissociation by competitor DNA, as well as by salt, Sarkosyl, and heparin. The effects of these inhibitory agents on transcription complex formation suggest that they target different steps in the assembly pathway.

摘要

我们通过非变性凝胶电泳解析了痘苗病毒编码的RNA聚合酶转录早期基因过程中的两个中间体。包含痘苗病毒早期转录因子(VETF)的聚合酶全酶形成了VETF与启动子结合的复合物,这是通向形成稳定三元延伸复合物途径的第一步。镁离子可刺激VETF-DNA复合物的形成,但不受核苷三磷酸的影响。未检测到RNA聚合酶与DNA形成的稳定二元复合物。凝胶稳定的聚合酶-DNA复合物的组装取决于允许RNA合成的条件。核苷酸缺失实验表明,在三元复合物稳定之前,至少必须合成一个四聚体RNA。RNA分析表明,含有20个核苷酸长新生转录本的复合物是稳定且有活性的。三元复合物的形成需要可水解的ATP。这与Broyles(S. S. Broyles,J. Biol. Chem. 266:15545-15548,1991)提出的VETF的ATPase活性在DNA结合后的步骤中起关键作用相一致。三元复合物一旦形成,就对竞争DNA以及盐、 Sarkosyl和肝素的解离具有抗性。这些抑制剂对转录复合物形成的影响表明它们靶向组装途径中的不同步骤。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/6fec/241057/c2a90d8cace3/jvirol00037-0396-a.jpg

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