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增强子启动使 Notch 信号能够快速持续地引发转录反应。

Enhancer Priming Enables Fast and Sustained Transcriptional Responses to Notch Signaling.

机构信息

Department of Physiology, Development and Neuroscience, University of Cambridge, Downing Street, Cambridge CB2 3DY, UK.

Biophysics Graduate Group, UC Berkeley, Berkeley, CA 94720, USA.

出版信息

Dev Cell. 2019 Aug 19;50(4):411-425.e8. doi: 10.1016/j.devcel.2019.07.002. Epub 2019 Aug 1.

Abstract

Information from developmental signaling pathways must be accurately decoded to generate transcriptional outcomes. In the case of Notch, the intracellular domain (NICD) transduces the signal directly to the nucleus. How enhancers decipher NICD in the real time of developmental decisions is not known. Using the MS2-MCP system to visualize nascent transcripts in single cells in Drosophila embryos, we reveal how two target enhancers read Notch activity to produce synchronized and sustained profiles of transcription. By manipulating the levels of NICD and altering specific motifs within the enhancers, we uncover two key principles. First, increased NICD levels alter transcription by increasing duration rather than frequency of transcriptional bursts. Second, priming of enhancers by tissue-specific transcription factors is required for NICD to confer synchronized and sustained activity; in their absence, transcription is stochastic and bursty. The dynamic response of an individual enhancer to NICD thus differs depending on the cellular context.

摘要

发育信号通路的信息必须被准确解码,以产生转录结果。在 Notch 的情况下,细胞内结构域(NICD)将信号直接转导到细胞核。目前尚不清楚增强子如何在发育决策的实时过程中解读 NICD。我们利用 MS2-MCP 系统在果蝇胚胎的单细胞中可视化新生转录本,揭示了两个靶增强子如何读取 Notch 活性以产生转录的同步和持续模式。通过操纵 NICD 的水平和改变增强子内的特定基序,我们揭示了两个关键原则。首先,增加 NICD 水平通过增加转录的持续时间而不是转录爆发的频率来改变转录。其次,组织特异性转录因子对增强子的启动对于 NICD 赋予同步和持续的活性是必需的;在它们不存在的情况下,转录是随机和爆发性的。因此,单个增强子对 NICD 的动态反应取决于细胞环境。

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