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Alternative cleavage and polyadenylation in spermatogenesis connects chromatin regulation with post-transcriptional control

机译:精子发生中的选择性切割和聚腺苷酸化将染色质调控与转录后调控联系起来

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Most mammalian genes display alternative cleavage and polyadenylation (APA). Previous studies have indicated preferential expression of APA isoforms with short 3’ untranslated regions (3’UTRs) in testes. By deep sequencing of the 3’ end region of poly(A)?+?transcripts, we report widespread shortening of 3’UTR through APA during the first wave of spermatogenesis in mouse, with 3’UTR size being the shortest in spermatids. Using genes without APA as a control, we show that shortening of 3’UTR eliminates destabilizing elements, such as U-rich elements and transposable elements, which appear highly potent during spermatogenesis. We additionally found widespread regulation of APA events in introns and exons that can affect the coding sequence of transcripts and global activation of antisense transcripts upstream of the transcription start site, suggesting modulation of splicing and initiation of transcription during spermatogenesis. Importantly, genes that display significant 3’UTR shortening tend to have functions critical for further sperm maturation, and testis-specific genes display greater 3’UTR shortening than ubiquitously expressed ones, indicating functional relevance of APA to spermatogenesis. Interestingly, genes with shortened 3’UTRs tend to have higher RNA polymerase II and H3K4me3 levels in spermatids as compared to spermatocytes, features previously known to be associated with open chromatin state. Our data suggest that open chromatin may create a favorable cis environment for 3’ end processing, leading to global shortening of 3’UTR during spermatogenesis. mRNAs with shortened 3’UTRs are relatively stable thanks to evasion of powerful mRNA degradation mechanisms acting on 3’UTR elements. Stable mRNAs generated in spermatids may be important for protein production at later stages of sperm maturation, when transcription is globally halted.
机译:大多数哺乳动物基因显示出替代的切割和聚腺苷酸化(APA)。先前的研究表明,APA亚型在睾丸中具有短3'非翻译区(3'UTR)的优先表达。通过对poly(A)++转录物的3'末端区域进行深度测序,我们报道了在小鼠第一次生精过程中,通过APA普遍缩短了3'UTR的缩短,其中3'UTR的大小是精子中最短的。使用不含APA的基因作为对照,我们显示3'UTR的缩短消除了不稳定因素,例如富含U元素和转座因子,这些元素在精子发生过程中表现出很高的效力。我们还发现内含子和外显子中APA事件的广泛调控会影响转录物的编码序列和转录起始位点上游的反义转录物的整体激活,这提示精子发生过程中剪接和转录起始的调控。重要的是,显示3'UTR明显缩短的基因往往具有对进一步精子成熟至关重要的功能,而睾丸特异性基因显示的3'UTR缩短比普遍表达的基因更大,这表明APA与精子发生功能相关。有趣的是,与精子细胞相比,具有3'UTR缩短的基因在精子中倾向于具有更高的RNA聚合酶II和H3K4me3水平,这是以前已知与开放染色质状态相关的特征。我们的数据表明,开放的染色质可能为3'末端加工创造有利的顺式环境,从而导致生精过程中3'UTR的全球缩短。由于避免了作用于3’UTR元件的强大的mRNA降解机制,具有3’UTR缩短的mRNA相对稳定。当转录全面停止时,精子中产生的稳定mRNA对于精子成熟后期的蛋白质生产可能很重要。

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