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了解配体结合对雌激素受体α-DNA复合物构象的影响:结合耗散型石英晶体微天平与表面等离子体共振的研究

Understanding ligand binding effects on the conformation of estrogen receptor alpha-DNA complexes: a combinational quartz crystal microbalance with dissipation and surface plasmon resonance study.

作者信息

Peh Wendy Y X, Reimhult Erik, Teh Huey Fang, Thomsen Jane S, Su Xiaodi

机构信息

Institute of Materials Research and Engineering, Singapore 117602.

出版信息

Biophys J. 2007 Jun 15;92(12):4415-23. doi: 10.1529/biophysj.106.099382. Epub 2007 Mar 23.

DOI:10.1529/biophysj.106.099382
PMID:17384075
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC1877774/
Abstract

Estrogen receptors are ligand-activated transcription factors that regulate gene expression by binding to specific DNA sequences. To date, the effect of ligands on the conformation of estrogen receptor alpha (ERalpha)-DNA complex remains a poorly understood issue. In our study, we are introducing the quartz crystal microbalance with dissipation monitoring (QCM-D) as a new alternative to study the conformational differences in protein-DNA complexes. Specifically, we have used QCM-D, in combination with surface plasmon resonance (SPR) spectroscopy, to monitor the binding of ERalpha to a specific DNA (estrogen response element, ERE) and a nonspecific DNA in the presence of either the agonist ligand, 17b-estradiol, the partial antagonist ligand, 4-hydroxytamoxifen, or vehicle alone. Both with presence and absence of ligand, the specific ERalpha-ERE complexes are observed to adopt a more compact conformation compared to nonspecific complexes. This observation is well correlated to the biophysical changes occurring during protein-DNA interaction shown by past structural and mechanism studies. Notably, pretreatment of ERalpha with E2 and 4OHT affects not only the viscoelasticity and conformation of the protein-DNA complex but also ERalpha binding capacity to immobilized ERE. These results affirm that ligands have remarkable effects on ERalpha-DNA complexes. Understanding these effects will provide insight into how ligand binding promotes subsequent events required for gene transcription.

摘要

雌激素受体是配体激活的转录因子,通过与特定DNA序列结合来调节基因表达。迄今为止,配体对雌激素受体α(ERα)-DNA复合物构象的影响仍是一个了解甚少的问题。在我们的研究中,我们引入了带耗散监测的石英晶体微天平(QCM-D)作为研究蛋白质-DNA复合物构象差异的新方法。具体而言,我们使用QCM-D结合表面等离子体共振(SPR)光谱,在存在激动剂配体17β-雌二醇、部分拮抗剂配体4-羟基他莫昔芬或仅使用溶剂的情况下,监测ERα与特定DNA(雌激素反应元件,ERE)和非特异性DNA的结合。无论有无配体,与非特异性复合物相比,特异性ERα-ERE复合物均呈现出更紧密的构象。这一观察结果与过去结构和机制研究中蛋白质-DNA相互作用过程中发生的生物物理变化密切相关。值得注意的是,用E2和4OHT对ERα进行预处理不仅会影响蛋白质-DNA复合物的粘弹性和构象,还会影响ERα与固定化ERE的结合能力。这些结果证实配体对ERα-DNA复合物有显著影响。了解这些影响将有助于深入了解配体结合如何促进基因转录所需的后续事件。

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