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首页> 外文期刊>BMC Genomics >The Drosophila early ovarian transcriptome provides insight to the molecular causes of recombination rate variation across genomes
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The Drosophila early ovarian transcriptome provides insight to the molecular causes of recombination rate variation across genomes

机译:果蝇早期卵巢转录组提供洞察跨基因组重组率变异的分子原因。

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Background Evidence in yeast indicates that gene expression is correlated with recombination activity and double-strand break (DSB) formation in some hotspots. Studies of nucleosome occupancy in yeast and mice also suggest that open chromatin influences the formation of DSBs. In Drosophila melanogaster, high-resolution recombination maps show an excess of DSBs within annotated transcripts relative to intergenic sequences. The impact of active transcription on recombination landscapes, however, remains unexplored in a multicellular organism. We then investigated the transcription profile during early meiosis in D. melanogaster females to obtain a glimpse at the relevant transcriptional dynamics during DSB formation, and test the specific hypothesis that DSBs preferentially target transcriptionally active genomic regions. Results Our study of transcript profiles of early- and late-meiosis using mRNA-seq revealed, 1) significant differences in gene expression, 2) new genes and exons, 3) parent-of-origin effects on transcription in early-meiosis stages, and 4) a nonrandom genomic distribution of transcribed genes. Importantly, genomic regions that are more actively transcribed during early meiosis show higher rates of recombination, and we ruled out DSB preference for genic regions that are not transcribed. Conclusions Our results provide evidence in a multicellular organism that transcription during the initial phases of meiosis increases the likelihood of DSB and give insight into the molecular determinants of recombination rate variation across the D. melanogaster genome. We propose that a model where variation in gene expression plays a role altering the recombination landscape across the genome could provide a molecular, heritable and plastic mechanism to observed patterns of recombination variation, from the high level of intra-specific variation to the known influence of environmental factors and stress conditions.
机译:背景技术酵母中的证据表明,基因表达与某些热点中的重组活性和双链断裂(DSB)形成相关。酵母和小鼠中核小体占有率的研究还表明,开放的染色质会影响DSB的形成。在果蝇中,高分辨率重组图显示了注释的转录本中相对于基因间序列而言过量的DSB。然而,在多细胞生物中,主动转录对重组景观的影响尚待探索。然后,我们调查了D. melanogaster雌性减数分裂早期的转录过程,以了解DSB形成过程中的相关转录动力学,并测试了DSB优先靶向转录活性基因组区域的特定假设。结果我们使用mRNA-seq对减数分裂早期和减数分裂的转录谱进行的研究表明:1)基因表达的显着差异; 2)新基因和外显子; 3)母本对减数分裂早期转录的影响, 4)转录基因的非随机基因组分布。重要的是,减数分裂早期转录活跃的基因组区域显示出更高的重组率,我们排除了DSB对未转录的基因区域的偏好。结论我们的结果提供了在多细胞生物中的证据,即减数分裂初始阶段的转录增加了DSB的可能性,并深入了解了黑​​腹果蝇基因组中重组率变异的分子决定因素。我们建议一个模型,其中基因表达的变化起着改变整个基因组重组格局的作用,可以为观察到的重组变异模式提供分子,遗传和塑性机制,从高水平的种内变异到已知的杂种优势。环境因素和压力条件。

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