首页> 外文期刊>Journal of Biophysical and Biochemical Cytology >MEIS homeodomain proteins facilitate PARP1/ARTD1-mediated eviction of histone H1
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MEIS homeodomain proteins facilitate PARP1/ARTD1-mediated eviction of histone H1

机译:MEIS同源域蛋白促进PARP1 / ARTD1介导的组蛋白H1的逐出

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Pre–B-cell leukemia homeobox (PBX) and myeloid ecotropic viral integration site (MEIS) proteins control cell fate decisions in many physiological and pathophysiological contexts, but how these proteins function mechanistically remains poorly defined. Focusing on the first hours of neuronal differentiation of adult subventricular zone–derived stem/progenitor cells, we describe a sequence of events by which PBX-MEIS facilitates chromatin accessibility of transcriptionally inactive genes: In undifferentiated cells, PBX1 is bound to the H1-compacted promoter/proximal enhancer of the neuron-specific gene doublecortin (Dcx) . Once differentiation is induced, MEIS associates with chromatin-bound PBX1, recruits PARP1/ARTD1, and initiates PARP1-mediated eviction of H1 from the chromatin fiber. These results for the first time link MEIS proteins to PARP-regulated chromatin dynamics and provide a mechanistic basis to explain the profound cellular changes elicited by these proteins.
机译:在许多生理和病理生理情况下,前B细胞白血病同源盒(PBX)和髓性嗜性病毒整合位点(MEIS)蛋白可控制细胞命运的决定,但这些蛋白如何以机械方式起作用仍然不清楚。着眼于成人脑室下区域衍生的干/祖细胞的神经元分化的最初几个小时,我们描述了一系列事件,PBX-MEIS通过这些事件促进转录不活跃基因的染色质可及性:在未分化的细胞中,PBX1与H1致密化结合神经元特异性基因doublecortin(Dcx)的启动子/近端增强子。诱导分化后,MEIS与结合染色质的PBX1结合,募集PARP1 / ARTD1,并启动PARP1介导的从染色质纤维中驱逐H1。这些结果首次将MEIS蛋白与PARP调节的染色质动力学联系起来,并为解释这些蛋白引起的深刻细胞变化提供了机理基础。

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