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Reciprocal regulation of chromatin state and architecture by HOTAIRM1 contributes to temporal collinear HOXA gene activation

机译:HOTAIRM1对染色质状态和结构的相互调节有助于时间共线HOXA基因激活

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摘要

Thousands of long non-coding RNAs (lncRNAs) have been identified in mammals, many of which represent important regulators of gene expression. However, the mechanisms used by lncRNAs to control transcription remain largely uncharacterized. Here, we report on HOTAIRM1, a promising lncRNA biomarker in leukemia and solid tumors. We find that HOTAIRM1 contributes to three-dimensional chromatin organization changes required for the temporal collinear activation of HOXA genes. We show that distinct HOTAIRM1 variants preferentially associate with either UTX/MLL or PRC2 complexes to modulate the levels of activating and silencing marks at the bivalent domain. HOTAIRM1 contributes to physical dissociation of chromatin loops at the cluster proximal end, which delays recruitment of the histone demethylase UTX and transcription of central HOXA genes. Interestingly, we find overall proximal HOXA gene activation without chromatin conformation changes by HOTAIRM1 in a different cell type. Our results reveal a previously unappreciated relationship between chromatin structure, architecture and lncRNA function.
机译:在哺乳动物中已经鉴定出数千种长的非编码RNA(lncRNA),其中许多代表了重要的基因表达调节剂。但是,lncRNAs用于控制转录的机制在很大程度上尚未阐明。在这里,我们报道了HOTAIRM1,它是白血病和实体瘤中一种有前途的lncRNA生物标志物。我们发现HOTAIRM1有助于HOXA基因的时间共线激活所需的三维染色质组织变化。我们显示,不同的HOTAIRM1变异体优先与UTX / MLL或PRC2复合物相关联,以调节在二价域激活和沉默标记的水平。 HOTAIRM1有助于群集近端染色质环的物理解离,这会延迟组蛋白脱甲基酶UTX的募集和中央HOXA基因的转录。有趣的是,我们发现在不同的细胞类型中,整个近端HOXA基因的激活没有被HOTAIRM1染色质构象改变。我们的研究结果揭示了染色质结构,结构与lncRNA功能之间以前未知的关系。

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