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经典 Wnt 信号通路中的二元转录调控。

Two-Element Transcriptional Regulation in the Canonical Wnt Pathway.

机构信息

Division of Biology and Biological Engineering, California Institute of Technology, Pasadena, CA 91125, USA.

Department of Physics and Department of Molecular Biology, University of California, San Diego, La Jolla, CA 92093, USA.

出版信息

Curr Biol. 2017 Aug 7;27(15):2357-2364.e5. doi: 10.1016/j.cub.2017.06.037. Epub 2017 Jul 27.

Abstract

The canonical Wnt pathway regulates numerous fundamental processes throughout development and adult physiology and is often disrupted in diseases [1-4]. Signal in the pathway is transduced by β-catenin, which in complex with Tcf/Lef regulates transcription. Despite the many processes that the Wnt pathway governs, β-catenin acts primarily on a single cis element in the DNA, the Wnt-responsive element (WRE), at times potentiated by a nearby Helper site. In this study, working with Xenopus, mouse, and human systems, we identified a cis element, distinct from WRE, upon which β-catenin and Tcf act. The element is 11 bp long, hundreds of bases apart from the WRE, and exhibits a suppressive effect. In Xenopus patterning, loss of the 11-bp negative regulatory elements (11-bp NREs) broadened dorsal expression of siamois. In mouse embryonic stem cells, genomic deletion of the 11-bp NREs in the promoter elevated Brachyury expression. This reveals a previously unappreciated mechanism within the Wnt pathway, where gene response is not only driven by WREs but also tuned by 11-bp NREs. Using electrophoretic mobility shift assay (EMSA) and chromatin immunoprecipitation (ChIP), we found evidence for the NREs binding to β-catenin and Tcf-suggesting a dual action by β-catenin as a signal and a feedforward sensor. Analyzing β-catenin ChIP sequencing in human cells, we found the 11-bp NREs co-localizing with the WRE in 45%-71% of the peaks, suggesting a widespread role for the mechanism. This study presents an example of a more complex cis regulation by a signaling pathway, where a signal is processed through two distinct cis elements in a gene circuitry.

摘要

经典的 Wnt 通路调节着发育和成人生理学过程中的众多基本过程,并且经常在疾病中被破坏[1-4]。该通路中的信号由β-catenin 转导,β-catenin 与 Tcf/Lef 形成复合物,调节转录。尽管 Wnt 通路调控着许多过程,但β-catenin 主要作用于 DNA 中的单个顺式元件,即 Wnt 反应元件(WRE),有时在附近的辅助位点的增强下发挥作用。在这项使用 Xenopus、小鼠和人类系统的研究中,我们确定了一个不同于 WRE 的顺式元件,β-catenin 和 Tcf 可以在其上发挥作用。该元件长 11bp,与 WRE 相距数百个碱基,具有抑制作用。在 Xenopus 模式形成中,11-bp 负调控元件(11-bp NREs)的缺失使 siamois 的背侧表达变宽。在小鼠胚胎干细胞中,启动子中 11-bp NREs 的基因组缺失会提高 Brachyury 的表达。这揭示了 Wnt 通路中的一种先前未被认识到的机制,即基因反应不仅由 WREs 驱动,还由 11-bp NREs 调节。通过电泳迁移率变动分析(EMSA)和染色质免疫沉淀(ChIP),我们发现 NREs 与 β-catenin 和 Tcf 结合的证据,这表明 β-catenin 作为信号和前馈传感器具有双重作用。分析人类细胞中的β-catenin ChIP 测序,我们发现 11-bp NREs 在 45%-71%的峰中与 WRE 共定位,这表明该机制具有广泛的作用。本研究提供了一个信号通路通过两个不同的顺式元件在基因电路中处理信号的更复杂的顺式调控的例子。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/41c1/5557293/74f82d032825/nihms886539f1.jpg

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