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T7 RNA 聚合酶延伸复合物的结构与运动

T7 RNA polymerase elongation complex structure and movement.

作者信息

Huang J, Sousa R

机构信息

Department of Biochemistry, University of Texas Health Sciences Center, 7703 Floyd Curl Drive, San Antonio, TX 78284-7760, USA.

出版信息

J Mol Biol. 2000 Oct 27;303(3):347-58. doi: 10.1006/jmbi.2000.4150.

Abstract

We have characterized T7RNAP elongation complexes (ECs) halted at different positions on a single template using a combination of digestion with exonuclease III, lambda exonuclease, RNAse T1, and treatment with KMnO(4). Our results indicate that the transcription bubble is approximately nine bases long and that the RNA:DNA hybrid is 7-8 bp in size. An additional four to six bases of RNA immediately 5' to the hybrid interact with the RNAP, probably with a site on the N-terminal domain. When ECs with transcripts of different length were probed in the presence or absence of the incoming NTP we found that the position of the EC on the template and the RNA shifted downstream upon NTP binding. NTP binding also restricted the lateral mobility of the complex on the template. Our results indicate that, in the absence of bound NTP, the RNAP is relatively free to slide on the template around a position that usually lies one to two bases upstream of the position from which NTP binding and bond formation occur. NTP binding stabilizes the RNAP in the post-translocated position and keeps it from sliding upstream, either due directly to RNAP:NTP:template interactions, or to an isomerization which causes the fingers subdomain of the RNAP to clamp down on the downstream end of the template strand.

摘要

我们使用核酸外切酶III、λ核酸外切酶、核糖核酸酶T1消化以及高锰酸钾处理相结合的方法,对在单个模板上不同位置停滞的T7 RNA聚合酶延伸复合物(ECs)进行了表征。我们的结果表明,转录泡大约有9个碱基长,RNA:DNA杂交体大小为7 - 8个碱基对。杂交体5'端紧邻的另外4至6个RNA碱基与RNA聚合酶相互作用,可能是与N端结构域上的一个位点相互作用。当在有或无进入的核苷三磷酸(NTP)的情况下探测具有不同长度转录本的ECs时,我们发现模板上EC的位置和RNA在NTP结合后向下游移动。NTP结合还限制了复合物在模板上的横向移动。我们的结果表明,在没有结合NTP的情况下,RNA聚合酶相对自由地在模板上围绕一个通常位于NTP结合和键形成位置上游一到两个碱基的位置滑动。NTP结合使RNA聚合酶在后易位位置稳定,并阻止其向上游滑动,这要么是由于RNA聚合酶:NTP:模板的直接相互作用,要么是由于一种异构化作用,该异构化作用导致RNA聚合酶的指状亚结构域夹住模板链的下游末端。

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