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先驱因子Foxa2在核受体FXR的配体依赖性激活中介导染色质构象变化。

Pioneer factor Foxa2 mediates chromatin conformation changes in ligand-dependent activation of nuclear receptor FXR.

作者信息

Hao Yi, Han Lu, Wu Anqi, Bochkis Irina M

出版信息

bioRxiv. 2023 Mar 8:2023.03.06.531297. doi: 10.1101/2023.03.06.531297.

Abstract

Activation of nuclear receptors, a family of ligand-dependent transcription factors, is used extensively in development of drug targets. We have previously shown that pioneer factor Foxa2 opens chromatin for binding of nuclear receptors FXR and LXRα during acute ligand activation. FXR is activated by bile acids and deletion of Foxa2 in the liver results in intrahepatic cholestasis. We hypothesized that Foxa2 also enables chromatin conformational changes during ligand activation. We performed Foxa2 HiChIP to assess Foxa2-dependent long-range interactions in mouse livers treated with either vehicle control or FXR agonist GW4064. HiChIP contact analysis shows that global chromatin interactions are dramatically increased during FXR activation. Ligand-treated livers exhibit extensive redistribution of topological associated domains (TAD and substantial increase in Foxa2-anchored loops, suggesting Foxa2 is involved in dynamic chromatin conformational changes. We demonstrate that chromatin conformation, including genome-wide interactions, TADs, intra-chromosomal and inter-chromosomal Foxa2-anchored loops, drastically changes upon addition of FXR agonist. Hence, we determine a novel role for Foxa2 in enabling these conformational changes, extending its function in bile acid metabolism.

摘要

核受体是一类依赖配体的转录因子家族,其激活在药物靶点开发中被广泛应用。我们之前已经表明,先驱因子Foxa2在急性配体激活过程中打开染色质,以供核受体FXR和LXRα结合。FXR由胆汁酸激活,肝脏中Foxa2的缺失会导致肝内胆汁淤积。我们推测Foxa2在配体激活过程中也能使染色质构象发生变化。我们进行了Foxa2 HiChIP实验,以评估在用载体对照或FXR激动剂GW4064处理的小鼠肝脏中依赖Foxa2的远程相互作用。HiChIP接触分析表明,在FXR激活过程中,整体染色质相互作用显著增加。用配体处理的肝脏表现出拓扑相关结构域(TAD)的广泛重新分布以及Foxa2锚定环的大量增加,这表明Foxa2参与了动态染色质构象变化。我们证明,加入FXR激动剂后,染色质构象,包括全基因组相互作用、TAD、染色体内和染色体间的Foxa2锚定环,会发生剧烈变化。因此,我们确定了Foxa2在促成这些构象变化中的新作用,扩展了其在胆汁酸代谢中的功能。

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