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LacI-DNA-IPTG 环:单分子 FRET 研究构象之间的平衡。

LacI-DNA-IPTG loops: equilibria among conformations by single-molecule FRET.

机构信息

Department of Chemistry and Biochemistry, University of Maryland, College Park, Maryland 20742, USA.

出版信息

J Phys Chem B. 2013 Apr 25;117(16):4713-22. doi: 10.1021/jp308930c. Epub 2013 Feb 13.

DOI:10.1021/jp308930c
PMID:23406418
Abstract

The E. coli Lac repressor (LacI) tetramer binds simultaneously to a promoter-proximal DNA binding site (operator) and an auxiliary operator, resulting in a DNA loop, which increases repression efficiency. Induction of the lac operon by allolactose reduces the affinity of LacI for DNA, but induction does not completely prevent looping in vivo. Our previous work on the conformations of LacI loops used a hyperstable model DNA construct, 9C14, that contains a sequence directed bend flanked by operators. Single-molecule fluorescence resonance energy transfer (SM-FRET) on a dual fluorophore-labeled LacI-9C14 loop showed that it adopts a single, stable, high-FRET V-shaped LacI conformation. Ligand-induced changes in loop geometry can affect loop stability, and the current work assesses loop population distributions for LacI-9C14 complexes containing the synthetic inducer IPTG. SM-FRET confirms that the high-FRET LacI-9C14 loop is only partially destabilized by saturating IPTG. LacI titration experiments and FRET fluctuation analysis suggest that the addition of IPTG induces loop conformational dynamics and re-equilibration between loop population distributions that include a mixture of looped states that do not exhibit high-efficiency FRET. The results show that repression by looping even at saturating IPTG should be considered in models for regulation of the operon. We propose that persistent DNA loops near the operator function biologically to accelerate rerepression upon exhaustion of inducer.

摘要

大肠杆菌 Lac 阻遏物(LacI)四聚体同时结合到启动子近端 DNA 结合位点(操纵子)和辅助操纵子上,形成 DNA 环,从而提高抑制效率。别乳糖诱导 lac 操纵子会降低 LacI 与 DNA 的亲和力,但诱导并不能完全阻止体内环化。我们之前关于 LacI 环构象的工作使用了一种超稳定的模型 DNA 构建体 9C14,它包含一个序列指导的弯曲,两侧是操纵子。双荧光标记的 LacI-9C14 环上的单分子荧光共振能量转移(SM-FRET)表明,它采用了一种单一、稳定、高 FRET 的 V 形 LacI 构象。环几何形状的配体诱导变化会影响环的稳定性,目前的工作评估了含有合成诱导物 IPTG 的 LacI-9C14 复合物的环种群分布。SM-FRET 证实,高 FRET LacI-9C14 环仅部分被饱和 IPTG 破坏。LacI 滴定实验和 FRET 波动分析表明,添加 IPTG 会诱导环构象动力学和环种群分布之间的再平衡,其中包括不表现出高效 FRET 的环化状态的混合物。结果表明,即使在饱和 IPTG 的情况下,通过环化进行的抑制作用也应在操纵子调控的模型中加以考虑。我们提出,在操纵子附近持续存在的 DNA 环在诱导物耗尽时有助于加速重新抑制。

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