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Mechanism of high-mobility group protein B enhancement of progesterone receptor sequence-specific DNA binding

机译:高迁移率族蛋白B增强孕酮受体序列特异性DNA结合的机制

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摘要

The DNA-binding domain (DBD) of progesterone receptor (PR) is bipartite containing a zinc module core that interacts with progesterone response elements (PRE), and a short flexible carboxyl terminal extension (CTE) that interacts with the minor groove flanking the PRE. The chromosomal high-mobility group B proteins (HMGB), defined as DNA architectural proteins capable of bending DNA, also function as auxiliary factors that increase the DNA-binding affinity of PR and other steroid receptors by mechanisms that are not well defined. Here we show that the CTE of PR contains a specific binding site for HMGB that is required for stimulation of PR-PRE binding, whereas the DNA architectural properties of HMGB are dispensable. Specific PRE DNA inhibited HMGB binding to the CTE, indicating that DNA and HMGB–CTE interactions are mutually exclusive. Exogenous CTE peptide increased PR-binding affinity for PRE as did deletion of the CTE. In a PR-binding site selection assay, A/T sequences flanking the PRE were enriched by HMGB, indicating that PR DNA-binding specificity is also altered by HMGB. We conclude that a transient HMGB–CTE interaction alters a repressive conformation of the flexible CTE enabling it to bind to preferred sequences flanking the PRE.
机译:孕酮受体(PR)的DNA结合结构域(DBD)是两部分的,包含与孕酮反应元件(PRE)相互作用的锌模块核心,和与PRE侧翼的小沟相互作用的短的柔性羧基末端延伸(CTE)。 。染色体高迁移率B组蛋白(HMGB)被定义为能够使DNA弯曲的DNA结构蛋白,并且还作为辅助因子发挥作用,其通过尚未明确定义的机制增加PR和其他类固醇受体的DNA结合亲和力。在这里,我们显示PR的CTE包含HMGB的特异性结合位点,这是刺激PR-PRE结合所必需的,而HMGB的DNA结构特性是可有可无的。特定的PRE DNA抑制HMGB与CTE的结合,表明DNA和HMGB-CTE相互作用是互斥的。外源CTE肽增加了对PRE的PR结合亲和力,CTE缺失也增加了。在PR结合位点选择测定中,PRE两侧的A / T序列被HMGB富集,表明PR DNA结合特异性也被HMGB改变。我们得出结论,短暂的HMGB-CTE相互作用改变了柔性CTE的阻抑构象,使其能够结合至PRE侧翼的优选序列。

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