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首页> 外文期刊>Nucleic Acids Research >Nucleosome regulatory dynamics in response to TGF beta
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Nucleosome regulatory dynamics in response to TGF beta

机译:响应TGFβ的核小体调节动力学

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Nucleosomes play important roles in a cell beyond their basal functionality in chromatin compaction. Their placement affects all steps in transcriptional regulation, from transcription factor (TF) binding to messenger ribonucleic acid (mRNA) synthesis. Careful profiling of their locations and dynamics in response to stimuli is important to further our understanding of transcriptional regulation by the state of chromatin. We measured nucleosome occupancy in human hepatic cells before and after treatment with transforming growth factor beta 1 (TGF beta 1), using massively parallel sequencing. With a newly developed method, SuMMIt, for precise positioning of nucleosomes we inferred dynamics of the nucleosomal landscape. Distinct nucleosome positioning has previously been described at transcription start site and flanking TF binding sites. We found that the average pattern is present at very few sites and, in case of TF binding, the double peak surrounding the sites is just an artifact of averaging over many loci. We systematically searched for depleted nucleosomes in stimulated cells compared to unstimulated cells and identified 24 318 loci. Depending on genomic annotation, 44-78% of them were over-represented in binding motifs for TFs. Changes in binding affinity were verified for HNF4 alpha by qPCR. Strikingly many of these loci were associated with expression changes, as measured by RNA sequencing
机译:核小体除了在染色质紧缩中的基本功能外,还在细胞中发挥重要作用。它们的位置会影响转录调控的所有步骤,从转录因子(TF)结合到信使核糖核酸(mRNA)合成。仔细分析它们的位置和动态响应刺激,对于进一步了解染色质状态对转录调控的理解非常重要。我们使用大规模平行测序法测量了转化生长因子β1(TGFβ1)处理之前和之后人类肝细胞中核小体的占有率。使用新开发的方法SuMMIt,可以精确定位核小体,从而推断出核小体景观的动态。先前已在转录起始位点和TF结合位点两侧描述了不同的核小体定位。我们发现平均模式出现在很少的位点上,并且在TF结合的情况下,位点周围的双峰只是在多个位点平均的伪像。我们系统地搜索与未刺激的细胞相比在刺激的细胞中的核小体减少,并确定了24 318个基因座。取决于基因组注释,其中44-78%在TF的结合基序中过量表达。通过qPCR验证了对于HNF4α的结合亲和力的变化。令人惊讶的是,这些位点中有许多与RNA测序所测的表达变化有关

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