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Essential role of paternal chromatin in the regulation of transcriptional activity during mouse preimplantation development

机译:父本染色质在小鼠植入前发育过程中调控转录活性的重要作用

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Several lines of evidence indicate that the formation of a transcriptionally repressive state during the two-cell stage in the preimplantation mouse embryo is superimposed on the activation of the embryonic genome. However, it is difficult to determine the profile of newly synthesized (nascent) RNA during this phase because large amounts of maternal RNA accumulate in maturing oocytes to support early development. Using 5-bromouridine-5′-triphosphate labeling of RNA, we have verified that nascent RNA synthesis was repressed between the two-cell and four-cell transition in normally fertilized but not in parthenogenetic embryos. Moreover, this repression was contributed by sperm (male) chromatin, which we confirmed by studying androgenetic embryos. The source of factors responsible for repressing nascent RNA production was investigated using different stages of sperm development. Fertilization with immature round spermatids resulted in a lower level of transcriptional activity than with ICSI at the two-cell stage, and this was consistent with further repression at the four-cell stage in the ICSI group. Finally, study on DNA replication and chromatin remodeling was performed using labeled histones H3 and H4 to differentiate between male and female pronuclei. The combination of male and female chromatin appeared to decrease nascent RNA production in the fertilized embryo. This study indicates that paternal chromatin is important in the regulation of transcriptional activity during mouse preimplantation development and that this capacity is acquired during spermiogenesis.
机译:几条证据表明,在植入前小鼠胚胎的两细胞阶段,转录抑制状态的形成与胚胎基因组的激活重叠。但是,在这一阶段很难确定新合成的(新生)RNA的概况,因为大量的母体RNA会积聚在成熟的卵母细胞中以支持早期发育。使用RNA的5-溴尿苷-5'-三磷酸酯标记,我们已经验证了在正常受精的单性生殖胚胎中两细胞和四细胞过渡之间新生的RNA合成被抑制。此外,这种抑制是由精子(雄性)染色质引起的,我们通过研究雄激素胚胎来证实了这一点。使用不同阶段的精子发育研究了抑制新生RNA产生的因素。不育的圆形精子受精导致的转录活性水平低于两细胞阶段的ICSI,这与ICSI组中四细胞阶段的进一步抑制相一致。最后,使用标记的组蛋白H3和H4进行了DNA复制和染色质重塑的研究,以区分雄性和雌性前核。男性和女性染色质的组合似乎减少了受精胚胎中新生RNA的产生。这项研究表明,父本染色质在小鼠植入前发育过程中对转录活性的调控很重要,并且这种能力是在精子发生过程中获得的。

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