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首页> 外文期刊>PLoS Genetics >Psip1/p52 regulates posterior Hoxa genes through activation of lncRNA Hottip
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Psip1/p52 regulates posterior Hoxa genes through activation of lncRNA Hottip

机译:Psip1 / p52通过激活lncRNA来调节后Hoxa基因

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Long noncoding RNAs (lncRNAs) have been implicated in various biological functions including the regulation of gene expression, however, the functionality of lncRNAs is not clearly understood and conflicting conclusions have often been reached when comparing different methods to investigate them. Moreover, little is known about the upstream regulation of lncRNAs. Here we show that the short isoform (p52) of a transcriptional co-activator—PC4 and SF2 interacting protein (Psip1), which is known to be involved in linking transcription to RNA processing, specifically regulates the expression of the lncRNA Hottip–located at the 5’ end of the Hoxa locus. Using both knockdown and knockout approaches we show that Hottip expression is required for activation of the 5’ Hoxa genes (Hoxa13 and Hoxa10/11) and for retaining Mll1 at the 5’ end of Hoxa. Moreover, we demonstrate that artificially inducing Hottip expression is sufficient to activate the 5’ Hoxa genes and that Hottip RNA binds to the 5’ end of Hoxa. By engineering premature transcription termination, we show that it is the Hottip lncRNA molecule itself, not just Hottip transcription that is required to maintains active expression of posterior Hox genes. Our data show a direct role for a lncRNA molecule in regulating the expression of developmentally-regulated mRNA genes in cis.
机译:长的非编码RNA(lncRNA)已牵涉到各种生物学功能,包括基因表达的调控,但是,lncRNA的功能尚不清楚,并且在比较不同的研究方法时常常得出相互矛盾的结论。此外,关于lncRNA的上游调控知之甚少。在这里,我们显示转录共激活因子— PC4和SF2相互作用蛋白(Psip1)的短同工型(p52),已知与转录与RNA加工有关,特别调节lncRNA Hottip的表达,其位于Hoxa基因座的5'末端。使用敲除和敲除方法,我们显示了Hottip表达对于激活5'Hoxa基因(Hoxa13和Hoxa10 / 11)以及将Mll1保留在Hoxa 5'末端是必需的。此外,我们证明了人工诱导Hottip表达足以激活5'Hoxa基因,并且Hottip RNA与Hoxa 5'末端结合。通过工程化过早的转录终止,我们表明,保持后Hox基因的主动表达所需的不仅仅是Hottip lncRNA分子本身,而不仅仅是Hottip转录。我们的数据显示了lncRNA分子在调节顺式中发育调控的mRNA基因表达中的直接作用。

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