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Dynamic exchange at regulatory elements during chromatin remodeling underlies assisted loading mechanism

机译:染色质重塑过程中调节元件的动态交换是辅助加载机制的基础

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摘要

The glucocorticoid receptor (GR), like other eukaryotic transcription factors, regulates gene expression by interacting with chromatinized DNA response elements. Photobleaching experiments in living cells indicate that receptors transiently interact with DNA on the time scale of seconds and predict that the response elements may be sparsely occupied on average. Here, we show that the binding of one receptor at the glucocorticoid response element (GRE) does not reduce the steady-state binding of another receptor variant to the same GRE. Mathematical simulations reproduce this noncompetitive state using short GR/GRE residency times and relatively long times between DNA binding events. At many genomic sites where GR binding causes increased chromatin accessibility, concurrent steady-state binding levels for the variant receptor are actually increased, a phenomenon termed assisted loading. Temporally sparse transcription factor-DNA interactions induce local chromatin reorganization, resulting in transient access for binding of secondary regulatory factors. PaperClip
机译:与其他真核转录因子一样,糖皮质激素受体(GR)通过与染色质DNA反应元件相互作用来调节基因表达。活细胞中的光漂白实验表明,受体在数秒的时间尺度上与DNA短暂相互作用,并预测平均而言反应元件可能稀疏。在这里,我们显示糖皮质激素反应元件(GRE)上一个受体的结合不会降低另一个受体变体与相同GRE的稳态结合。数学模拟使用较短的GR / GRE驻留时间和较长的DNA结合事件之间的时间来重现此非竞争状态。在GR结合导致染色质可及性增加的许多基因组位点,变异受体的同时稳态结合水平实际上增加了,这种现象称为辅助加载。暂时稀疏的转录因子与DNA的相互作用会引起局部染色质重组,从而导致瞬时进入二级调节因子的结合。回形针

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