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FOXA2 对于胰腺分化过程中的增强子起始是必需的。

FOXA2 Is Required for Enhancer Priming during Pancreatic Differentiation.

机构信息

Developmental Biology Program, Memorial Sloan Kettering Cancer Center, New York, NY 10065, USA; Weill Graduate School of Medical Sciences at Cornell University, New York, NY 10065, USA.

Weill Graduate School of Medical Sciences at Cornell University, New York, NY 10065, USA; Computational Biology Program, Memorial Sloan Kettering Cancer Center, New York, NY 10065, USA.

出版信息

Cell Rep. 2019 Jul 9;28(2):382-393.e7. doi: 10.1016/j.celrep.2019.06.034.

Abstract

Transcriptional regulatory mechanisms of lineage priming in embryonic development are largely uncharacterized because of the difficulty of isolating transient progenitor populations. Directed differentiation of human pluripotent stem cells (hPSCs) combined with gene editing provides a powerful system to define precise temporal gene requirements for progressive chromatin changes during cell fate transitions. Here, we map the dynamic chromatin landscape associated with sequential stages of pancreatic differentiation from hPSCs. Our analysis of chromatin accessibility dynamics led us to uncover a requirement for FOXA2, known as a pioneer factor, in human pancreas specification not previously shown from mouse knockout studies. FOXA2 knockout hPSCs formed reduced numbers of pancreatic progenitors accompanied by impaired recruitment of GATA6 to pancreatic enhancers. Furthermore, FOXA2 is required for proper chromatin remodeling and H3K4me1 deposition during enhancer priming. This work highlights the power of combining hPSC differentiation, genome editing, and computational genomics for discovering transcriptional mechanisms during development.

摘要

胚胎发育中谱系启动的转录调控机制在很大程度上尚未被阐明,因为难以分离瞬时祖细胞群体。人多能干细胞(hPSC)的定向分化与基因编辑相结合,为定义细胞命运转变过程中渐进性染色质变化的精确时间基因需求提供了一个强大的系统。在这里,我们绘制了人多能干细胞向胰腺分化的连续阶段相关的动态染色质图谱。我们对染色质可及性动态的分析使我们发现了 FOXA2 的作用,FOXA2 作为一种先驱因子,在以前的小鼠敲除研究中没有显示出对人类胰腺特化的要求。FOXA2 敲除的 hPSC 形成的胰腺祖细胞数量减少,同时 GATA6 招募到胰腺增强子的能力受损。此外,FOXA2 对于增强子启动过程中的正确染色质重塑和 H3K4me1 沉积是必需的。这项工作突出了结合 hPSC 分化、基因组编辑和计算基因组学来发现发育过程中的转录机制的强大功能。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/ba93/6636862/0c8dd4b732f6/nihms-1534202-f0002.jpg

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