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Disordered chromatin packing regulates phenotypic plasticity

机译:染色质填料紊乱调节表型可塑性

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Three-dimensional supranucleosomal chromatin packing plays a profound role in modulating gene expression by regulating transcription reactions through mechanisms such as gene accessibility, binding affinities, and molecular diffusion. Here, we use a computational model that integrates disordered chromatin packing (CP) with local macromolecular crowding (MC) to study how physical factors, including chromatin density, the scaling of chromatin packing, and the size of chromatin packing domains, influence gene expression. We computationally and experimentally identify a major role of these physical factors, specifically chromatin packing scaling, in regulating phenotypic plasticity, determining responsiveness to external stressors by influencing both intercellular transcriptional malleability and heterogeneity. Applying CPMC model predictions to transcriptional data from cancer patients, we identify an inverse relationship between patient survival and phenotypic plasticity of tumor cells.
机译:三维上核核糖囊染色质包装在通过调节转录反应通过诸如基因可访问性,结合亲和力和分子扩散的机制调节转录反应来调节基因表达。在这里,我们使用与局部大分子挤出(MC)整合有序染色质包装(CP)的计算模型,以研究物理因素如何,包括染色质密度,染色质填料的缩放,以及染色质包装结构域的大小,影响基因表达。我们在计算上并通过实验地确定这些物理因素,特别是染色质包装缩放,调节表型塑性,通过影响细胞间转录术和异质性来确定对外部压力源的反应性的主要作用。将CPMC模型预测应用于来自癌症患者的转录数据,我们确定患者存活和肿瘤细胞表型可塑性之间的反比关系。

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