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胚胎干细胞中的转录因子结合受DNA序列重复对称性的限制。

Transcription Factor Binding in Embryonic Stem Cells Is Constrained by DNA Sequence Repeat Symmetry.

作者信息

Goldshtein Matan, Mellul Meir, Deutch Gai, Imashimizu Masahiko, Takeuchi Koh, Meshorer Eran, Ram Oren, Lukatsky David B

机构信息

Avram and Stella Goldstein-Goren Department of Biotechnology Engineering, Ben-Gurion University of the Negev, Beer-Sheva, Israel.

Department of Biological Chemistry, The Institute of Life Sciences, The Hebrew University of Jerusalem, Jerusalem, Israel.

出版信息

Biophys J. 2020 Apr 21;118(8):2015-2026. doi: 10.1016/j.bpj.2020.02.009. Epub 2020 Feb 15.

Abstract

Transcription factor (TF) recognition is dictated by the underlying DNA motif sequence specific for each TF. Here, we reveal that DNA sequence repeat symmetry plays a central role in defining TF-DNA-binding preferences. In particular, we find that different TFs bind similar symmetry patterns in the context of different developmental layers. Most TFs possess dominant preferences for similar DNA repeat symmetry types. However, in some cases, preferences of specific TFs are changed during differentiation, suggesting the importance of information encoded outside of known motif regions. Histone modifications also exhibit strong preferences for similar DNA repeat symmetry patterns unique to each type of modification. Next, using an in vivo reporter assay, we show that gene expression in embryonic stem cells can be positively modulated by the presence of genomic and computationally designed DNA oligonucleotides containing identified nonconsensus-repetitive sequence elements. This supports the hypothesis that certain nonconsensus-repetitive patterns possess a functional ability to regulate gene expression. We also performed a solution NMR experiment to probe the stability of double-stranded DNA via imino proton resonances for several double-stranded DNA sequences characterized by different repetitive patterns. We suggest that such local stability might play a key role in determining TF-DNA binding preferences. Overall, our findings show that despite the enormous sequence complexity of the TF-DNA binding landscape in differentiating embryonic stem cells, this landscape can be quantitatively characterized in simple terms using the notion of DNA sequence repeat symmetry.

摘要

转录因子(TF)的识别取决于每个TF特有的潜在DNA基序序列。在此,我们揭示了DNA序列重复对称性在定义TF-DNA结合偏好方面起着核心作用。具体而言,我们发现在不同发育层的背景下,不同的TF结合相似的对称模式。大多数TF对相似的DNA重复对称类型具有主导偏好。然而,在某些情况下,特定TF的偏好在分化过程中会发生变化,这表明已知基序区域之外编码的信息很重要。组蛋白修饰对每种修饰类型特有的相似DNA重复对称模式也表现出强烈偏好。接下来,使用体内报告基因检测,我们表明胚胎干细胞中的基因表达可以通过含有已鉴定的非共识重复序列元件的基因组和计算设计的DNA寡核苷酸的存在而得到正向调节。这支持了这样一种假设,即某些非共识重复模式具有调节基因表达的功能能力。我们还进行了溶液核磁共振实验,通过亚氨基质子共振来探测几种具有不同重复模式特征的双链DNA序列的双链DNA稳定性。我们认为这种局部稳定性可能在确定TF-DNA结合偏好方面起关键作用。总体而言,我们的研究结果表明,尽管分化的胚胎干细胞中TF-DNA结合格局的序列复杂性极高,但使用DNA序列重复对称的概念可以简单地对这种格局进行定量表征。

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