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大肠杆菌环磷酸腺苷受体蛋白介导的转录激活。串联结合在启动子上的受体可发生协同相互作用。

Transcription activation by the Escherichia coli cyclic AMP receptor protein. Receptors bound in tandem at promoters can interact synergistically.

作者信息

Busby S, West D, Lawes M, Webster C, Ishihama A, Kolb A

机构信息

School of Biochemistry, University of Birmingham, U.K.

出版信息

J Mol Biol. 1994 Aug 19;241(3):341-52. doi: 10.1006/jmbi.1994.1511.

Abstract

Starting with a semi-synthetic Escherichia coli promoter with a binding site for the cyclic AMP receptor protein (CRP) centred between base-pairs 41 and 42 upstream from the transcription start site, a second upstream CRP-binding site, centred between base-pairs 90 and 91, was introduced. CRP binding to this second upstream site results in a several-fold greater stimulation of CRP-dependent transcription initiation, compared to activation at the starting promoter with just one CRP-binding site. Activation of transcription by the upstream CRP molecule is blocked by the HL159 substitution, suggesting that the upstream-bound CRP makes a direct contact with RNA polymerase. Footprinting experiments suggest that RNA polymerase contacts the promoter DNA between the two CRP-binding sites, most likely due to interactions involving the C-terminal part of the alpha subunit. Synergy between tandem bound CRP molecules in transcription activation requires that the two CRP-binding sites be separated by around 40 or 50 base-pairs, but is not found at intermediate spacings. An experiment in which the upstream CRP-binding site is replaced by a site for the related transcription factor, FNR, shows that heterologous synergistic interactions between FNR and CRP are possible.

摘要

从一个半合成的大肠杆菌启动子开始,该启动子具有一个环腺苷酸受体蛋白(CRP)结合位点,位于转录起始位点上游41和42碱基对之间的中心位置,引入了第二个上游CRP结合位点,位于90和91碱基对之间的中心位置。与仅具有一个CRP结合位点的起始启动子相比,CRP与这个第二个上游位点的结合导致对CRP依赖性转录起始的刺激增加了几倍。上游CRP分子对转录的激活被HL159取代所阻断,这表明上游结合的CRP与RNA聚合酶直接接触。足迹实验表明,RNA聚合酶在两个CRP结合位点之间与启动子DNA接触,这很可能是由于涉及α亚基C末端部分的相互作用。串联结合的CRP分子在转录激活中的协同作用要求两个CRP结合位点相隔约40或50个碱基对,但在中间间距时未发现协同作用。一项将上游CRP结合位点替换为相关转录因子FNR的位点的实验表明,FNR和CRP之间可能存在异源协同相互作用。

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