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A novel non-coding RNA lncRNA-JADE connects DNA damage signalling to histone H4 acetylation

机译:新型非编码RNA lncRNA-JADE将DNA损伤信号转导至组蛋白H4乙酰化

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摘要

A prompt and efficient DNA damage response (DDR) eliminates the detrimental effects of DNA lesions in eukaryotic cells. Basic and preclinical studies suggest that the DDR is one of the primary anti-cancer barriers during tumorigenesis. The DDR involves a complex network of processes that detect and repair DNA damage, in which long non-coding RNAs (lncRNAs), a new class of regulatory RNAs, may play an important role. In the current study, we identified a novel lncRNA, lncRNA-JADE, that is induced after DNA damage in an ataxia-telangiectasia mutated (ATM)-dependent manner. LncRNA-JADE transcriptionally activates Jade1, a key component in the HBO1 (human acetylase binding to ORC1) histone acetylation complex. Consequently, lncRNA-JADE induces histone H4 acetylation in the DDR. Markedly higher levels of lncRNA-JADE were observed in human breast tumours in comparison with normal breast tissues. Knockdown of lncRNA-JADE significantly inhibited breast tumour growth in vivo. On the basis of these results, we propose that lncRNA-JADE is a key functional link that connects the DDR to histone H4 acetylation, and that dysregulation of lncRNA-JADE may contribute to breast tumorigenesis.
机译:快速有效的DNA损伤反应(DDR)消除了真核细胞中DNA损伤的有害影响。基础和临床前研究表明,DDR是肿瘤发生过程中主要的抗癌屏障之一。 DDR包含检测和修复DNA损伤的复杂过程网络,其中长的非编码RNA(lncRNA)是一类新型的调控RNA,在其中可能发挥重要作用。在当前的研究中,我们确定了一种新型的lncRNA,即lncRNA-JADE,它在DNA损伤后以共济失调-毛细血管扩张突变(ATM)依赖性方式被诱导。 LncRNA-JADE转录激活Jade1,Jade1是HBO1(与ORC1结合的人乙酰化酶)组蛋白乙酰化复合物中的关键成分。因此,lncRNA-JADE在DDR中诱导组蛋白H4乙酰化。与正常乳腺组织相比,在人乳腺肿瘤中观察到的lncRNA-JADE水平明显更高。敲低lncRNA-JADE在体内显着抑制了乳腺肿瘤的生长。根据这些结果,我们认为lncRNA-JADE是将DDR连接至组蛋白H4乙酰化的关键功能性连接,而lncRNA-JADE的失调可能有助于乳腺癌的发生。

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