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Brahma regulates a specific trans-splicing event at the mod(mdg4) locus of Drosophila melanogaster

机译:梵天调节果蝇的mod(mdg4)基因座上的特定转拼事件。

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The mod(mdg4) locus of Drosophila melanogaster contains several transcription units encoded on both DNA strands. The mod(mdg4) pre-mRNAs are alternatively spliced, and a very significant fraction of the mature mod(mdg4) mRNAs are formed by trans-splicing. We have studied the transcripts derived from one of the anti-sense regions within the mod(mdg4) locus in order to shed light on the expression of this complex locus. We have characterized the expression of anti-sense mod(mdg4) transcripts in S2 cells, mapped their transcription start sites and cleavage sites, identified and quantified alternatively spliced transcripts, and obtained insight into the regulation of the mod(mdg4) trans-splicing. In a previous study, we had shown that the alternative splicing of some mod(mdg4) transcripts was regulated by Brahma (BRM), the ATPase subunit of the SWI/SNF chromatin-remodeling complex. Here we show, using RNA interference and overexpression of recombinant BRM proteins, that the levels of BRM affect specifically the abundance of a trans-spliced mod(mdg4) mRNA isoform in both S2 cells and larvae. This specific effect on trans-splicing is accompanied by a local increase in the density of RNA polymerase II and by a change in the phosphorylation state of the C-terminal domain of the large subunit of RNA polymerase II. Interestingly, the regulation of the mod(mdg4) splicing by BRM is independent of the ATPase activity of BRM, which suggests that the mechanism by which BRM modulates trans-splicing is independent of its chromatin-remodeling activity.
机译:果蝇的mod(mdg4)基因座包含两个DNA链上编码的几个转录单位。将mod(mdg4)pre-mRNA进行剪接,并通过反式剪接形成非常大部分的成熟mod(mdg4)mRNA。我们研究了源自mod(mdg4)基因座中反义区域之一的转录本,以阐明该复杂基因座的表达。我们已经表征了反义mod(mdg4)转录本在S2细胞中的表达,定位了它们的转录起始位点和切割位点,鉴定并量化了交替剪接的转录本,并获得了对mod(mdg4)反式剪接调控的见解。在先前的研究中,我们已经表明,某些mod(mdg4)转录本的选择性剪接受Brahma(BRM)(SWI / SNF染色质重塑复合体的ATPase亚基)调控。在这里我们显示,使用RNA干扰和重组BRM蛋白的过表达,BRM的水平特别影响S2细胞和幼虫中反式剪接的mod(mdg4)mRNA同工型的丰度。对反式剪接的这种特定作用伴随着RNA聚合酶II的密度的局部增加和RNA聚合酶II的大亚基的C末端结构域的磷酸化状态的改变。有趣的是,BRM对mod(mdg4)剪接的调节与BRM的ATPase活性无关,这表明BRM调节反式剪接的机制与其染色质重塑活性无关。

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