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Distinct regulatory programs establish widespread sex-specific alternative splicing in Drosophila melanogaster

机译:不同的监管计划在果蝇中建立了广泛的针对性别的选择性剪接

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摘要

In Drosophila melanogaster, female-specific expression of Sex-lethal (SXL) and Transformer (TRA) proteins controls sex-specific alternative splicing and/or translation of a handful of regulatory genes responsible for sexual differentiation and behavior. Recent findings in 2009 by Telonis-Scott et al. document widespread sex-biased alternative splicing in fruitflies, including instances of tissue-restricted sex-specific splicing. Here we report results arguing that some of these novel sex-specific splicing events are regulated by mechanisms distinct from those established by female-specific expression of SXL and TRA. Bioinformatic analysis of SXL/TRA binding sites, experimental analysis of sex-specific splicing in S2 and Kc cells lines and of the effects of SXL knockdown in Kc cells indicate that SXL-dependent and SXL-independent regulatory mechanisms coexist within the same cell. Additional determinants of sex-specific splicing can be provided by sex-specific differences in the expression of RNA binding proteins, including Hrp40/Squid. We report that sex-specific alternative splicing of the gene hrp40/squid leads to sex-specific differences in the levels of this hnRNP protein. The significant overlap between sex-regulated alternative splicing changes and those induced by knockdown of hrp40/squid and the presence of related sequence motifs enriched near subsets of Hrp40/Squid-regulated and sex-regulated splice sites indicate that this protein contributes to sex-specific splicing regulation. A significant fraction of sex-specific splicing differences are absent in germline-less tudor mutant flies. Intriguingly, these include alternative splicing events that are differentially spliced in tissues distant from the germline. Collectively, our results reveal that distinct genetic programs control widespread sex-specific splicing in Drosophila melanogaster.
机译:在果蝇中,雌性致死(SXL)和变压器(TRA)蛋白的女性特异性表达控制着负责性别分化和行为的少数调控基因的性别特异性交替剪接和/或翻译。 Telonis-Scott等人在2009年的最新发现。文献记载了在果蝇中普遍存在的性别偏见的选择性剪接,包括组织受限的性别特异性剪接的实例。在这里,我们报告的结果争论说,这些新颖的性别特异性剪接事件中的一些受与SXL和TRA的女性特异性表达所建立的机制不同的机制调控。 SXL / TRA结合位点的生物信息学分析,S2和Kc细胞系中性别特异性剪接的实验分析以及Kc细胞中SXL敲低的影响表明,SXL依赖性和SXL依赖性调节机制共存于同一细胞内。可以通过RNA结合蛋白(包括Hrp40 / Squid)的表达中的性别特异性差异来提供性别特异性剪接的其他决定因素。我们报告说,基因hrp40 / squid的性别特异性替代剪接导致该hnRNP蛋白水平的性别特异性差异。性别调控的可变剪接变化与hrp40 / squid的敲低诱导的相关性之间的显着重叠以及Hrp40 / Squid调控和性别调控的剪接位点附近子集附近丰富的相关序列基序的存在表明该蛋白有助于性别特异性拼接规则。无种系的都铎突变体蝇中不存在很大比例的性别特异性剪接差异。有趣的是,这些包括在远离种系的组织中差异剪接的替代剪接事件。总体而言,我们的结果表明,不同的遗传程序控制着果蝇中广泛的性别特异性剪接。

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