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转录因子FadR的酰基辅酶A依赖性调控的结构基础

The structural basis of acyl coenzyme A-dependent regulation of the transcription factor FadR.

作者信息

van Aalten D M, DiRusso C C, Knudsen J

机构信息

Wellcome Trust Biocentre, Division of Biological Chemistry and Molecular Microbiology, School of Life Sciences, University of Dundee, Dow Street, Dundee DD1 5EH, UK.

出版信息

EMBO J. 2001 Apr 17;20(8):2041-50. doi: 10.1093/emboj/20.8.2041.

Abstract

FadR is an acyl-CoA-responsive transcription factor, regulating fatty acid biosynthetic and degradation genes in Escherichia coli. The apo-protein binds DNA as a homodimer, an interaction that is disrupted by binding of acyl-COA: The recently described structure of apo-FadR shows a DNA binding domain coupled to an acyl-CoA binding domain with a novel fold, but does not explain how binding of the acyl-CoA effector molecule > 30 A away from the DNA binding site affects transcriptional regulation. Here, we describe the structures of the FadR-operator and FadR- myristoyl-CoA binary complexes. The FadR-DNA complex reveals a novel winged helix-turn-helix protein-DNA interaction, involving sequence-specific contacts from the wing to the minor groove. Binding of acyl-CoA results in dramatic conformational changes throughout the protein, with backbone shifts up to 4.5 A. The net effect is a rearrangement of the DNA binding domains in the dimer, resulting in a change of 7.2 A in separation of the DNA recognition helices and the loss of DNA binding, revealing the molecular basis of acyl-CoA-responsive regulation.

摘要

FadR是一种酰基辅酶A反应性转录因子,可调节大肠杆菌中的脂肪酸生物合成和降解基因。脱辅基蛋白以同二聚体形式结合DNA,这种相互作用会因酰基辅酶A的结合而被破坏:最近描述的脱辅基FadR结构显示,一个具有新颖折叠方式的DNA结合结构域与一个酰基辅酶A结合结构域相连,但并未解释距离DNA结合位点超过30埃的酰基辅酶A效应分子的结合如何影响转录调控。在此,我们描述了FadR-操纵基因和FadR-肉豆蔻酰辅酶A二元复合物的结构。FadR-DNA复合物揭示了一种新颖的带翼螺旋-转角-螺旋蛋白-DNA相互作用,涉及从翼到小沟的序列特异性接触。酰基辅酶A的结合导致整个蛋白质发生显著的构象变化,主链位移高达4.5埃。最终结果是二聚体中DNA结合结构域的重排,导致DNA识别螺旋之间的间距变化7.2埃并失去DNA结合能力,揭示了酰基辅酶A反应性调控的分子基础。

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