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Coordinated binding of NF-κB family members in the response of human cells to lipopolysaccharide

机译:NF-κB家族成员在人细胞对脂多糖反应中的协同结合

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The NF-κB family of transcription factors plays a critical role in numerous cellular processes, particularly the immune response. Our understanding of how the different NF-κB subunits act coor-dinately to regulate gene expression is based on a limited set of genes. We used genome-scale location analysis to identify targets of all five NF-κB proteins before and after stimulation of monocytic cells with bacterial lipopolysaccharide (LPS). In unstimulated cells, p50 and p52 bound to a large number of gene promoters that were also occupied by RNA polymerase II. After LPS stimulation, additional NF-κB subunits bound to these genes and to other genes. Genes that became bound by multiple NF-κB subunits were the most likely to show increases in RNA polymerase II occupancy and gene expression. This study identifies NF-κB target genes, reveals how the different NF-κB proteins coordinate their activity, and provides an initial map of the transcriptional regulatory network that underlies the host response to infection.
机译:NF-κB转录因子家族在许多细胞过程中,尤其是免疫反应中起着至关重要的作用。我们对不同的NF-κB亚基如何协同作用来调节基因表达的理解是基于有限的一组基因。我们使用基因组规模的位置分析来确定细菌脂多糖(LPS)刺激单核细胞之前和之后所有五个NF-κB蛋白的目标。在未刺激的细胞中,p50和p52与大量基因启动子结合,而这些基因启动子也被RNA聚合酶II占据。 LPS刺激后,其他NF-κB亚基与这些基因和其他基因结合。被多个NF-κB亚基结合的基因最有可能显示RNA聚合酶II占有率和基因表达的增加。这项研究鉴定了NF-κB靶基因,揭示了不同的NF-κB蛋白如何协调其活性,并提供了转录调控网络的初步图谱,该网络是宿主对感染的反应的基础。

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