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串联 DNA 重复序列在维持间充质特性中的协同作用。

Co-optation of Tandem DNA Repeats for the Maintenance of Mesenchymal Identity.

机构信息

Department of Experimental Oncology, European Institute of Oncology (IEO), Via Adamello 16, 20139 Milan, Italy.

Humanitas Clinical and Research Center, Via Manzoni 56, 20089 Rozzano, Milan, Italy.

出版信息

Cell. 2018 May 17;173(5):1150-1164.e14. doi: 10.1016/j.cell.2018.03.081. Epub 2018 Apr 26.

Abstract

Tandem repeats (TRs) are generated by DNA replication errors and retain a high level of instability, which in principle would make them unsuitable for integration into gene regulatory networks. However, the appearance of DNA sequence motifs recognized by transcription factors may turn TRs into functional cis-regulatory elements, thus favoring their stabilization in genomes. Here, we show that, in human cells, the transcriptional repressor ZEB1, which promotes the maintenance of mesenchymal features largely by suppressing epithelial genes and microRNAs, occupies TRs harboring dozens of copies of its DNA-binding motif within genomic loci relevant for maintenance of epithelial identity. The deletion of one such TR caused quasi-mesenchymal cancer cells to reacquire epithelial features, partially recapitulating the effects of ZEB1 gene deletion. These data demonstrate that the high density of identical motifs in TRs can make them suitable platforms for recruitment of transcriptional repressors, thus promoting their exaptation into pre-existing cis-regulatory networks.

摘要

串联重复序列 (TRs) 是由 DNA 复制错误产生的,并且保留了高度的不稳定性,这从原则上使它们不适合整合到基因调控网络中。然而,转录因子识别的 DNA 序列基序的出现可能会使 TR 成为功能性顺式调控元件,从而有利于它们在基因组中的稳定。在这里,我们表明,在人类细胞中,转录抑制因子 ZEB1 通过抑制上皮基因和 microRNAs 来促进间充质特征的维持,它占据了基因组中与维持上皮特征相关的基因座内含有数十个其 DNA 结合基序的 TR。删除这样一个 TR 会导致准间充质癌细胞重新获得上皮特征,部分重现了 ZEB1 基因缺失的效果。这些数据表明,TR 中相同基序的高密度可以使它们成为招募转录抑制因子的合适平台,从而促进它们被适应到预先存在的顺式调控网络中。

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