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Widespread transcript shortening through alternative polyadenylation in secretory cell differentiation

机译:通过分泌细胞分化中的替代聚腺苷酸化缩短的广泛成绩单

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摘要

Most eukaryotic genes produce alternative polyadenylation (APA) isoforms. Here we report that, unlike previously characterized cell lineages, differentiation of syncytiotrophoblast (SCT), a cell type critical for hormone production and secretion during pregnancy, elicits widespread transcript shortening through APA in 3'UTRs and in introns. This global APA change is observed in multiple in vitro trophoblast differentiation models, and in single cells from placentas at different stages of pregnancy. Strikingly, the transcript shortening is unrelated to cell proliferation, a feature previously associated with APA control, but instead accompanies increased secretory functions. We show that 3'UTR shortening leads to transcripts with higher mRNA stability, which augments transcriptional activation, especially for genes involved in secretion. Moreover, this mechanism, named secretion-coupled APA (SCAP), is also executed in B cell differentiation to plasma cells. Together, our data indicate that SCAP tailors the transcriptome during formation of secretory cells, boosting their protein production and secretion capacity.
机译:大多数真核基因产生替代的多腺苷酸(APA)同种型。在这里,我们报告说,与先前表征的细胞谱系不同,同性恋营养细胞(SCT)的分化,对妊娠期间对激素产生和分泌至关重要的细胞类型,引发了3'UTRS和内含子中的APA缩短的广泛成绩单。在多种体外滋养细胞分化模型中观察到这种全局APA变化,以及在怀孕的不同阶段的胎盘中的单细胞中。尖锐的是,转录物缩短与细胞增殖无关,先前与APA控制相关联的特征,而是伴随着增加的分泌功能。我们表明,3'UTR缩短导致具有较高mRNA稳定性的转录性,这增加了转录激活,特别是对于分泌中涉及的基因。此外,该机制名为分泌耦合APA(SCAP),也在B细胞分化中执行到等离子体细胞。在一起,我们的数据表明,在分泌细胞的形成期间,突然剪裁了转录组,促进其蛋白质产生和分泌能力。

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