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Zygotic Genome Activation Triggers the DNA Replication Checkpoint at the Midblastula Transition

机译:合子基因组激活在中胚层过渡期触发DNA复制检查点。

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A conserved feature of the midblastula transition (MBT) is a requirement for a functional DNA replication checkpoint to coordinate cell-cycle remodeling and zygotic genome activation (ZGA). We have investigated what triggers this checkpoint during Drosophila embryogenesis. We find that the magnitude of the checkpoint scales with the quantity of transcriptionally engaged DNA. Measuring RNA polymerase II (Pol II) binding at 20 min intervals over the course of ZGA reveals that the checkpoint coincides with widespread de novo recruitment of Pol II that precedes and does not require a functional checkpoint. This recruitment drives slowing or stalling of DNA replication at transcriptionally engaged loci. Reducing Pol II recruitment in zelda mutants both reduces replication stalling and bypasses the requirement for a functional checkpoint. This suggests a model where the checkpoint functions as a feedback mechanism to remodel the cell cycle in response to nascent ZGA.
机译:中胚层过渡(MBT)的保守特征是功能性DNA复制检查点需要协调细胞周期重塑和合子基因组激活(ZGA)的要求。我们调查了果蝇胚胎发生过程中触发此检查点的原因。我们发现,检查点的大小与转录参与的DNA的数量成比例。在ZGA的过程中,以20分钟的间隔测量RNA聚合酶II(Pol II)的结合表明,该检查点与之前且不需要功能检查点的广泛的Pol II从头募集相吻合。这种募集使转录参与的基因座处的DNA复制减慢或停滞。减少zelda突变体中Pol II的募集既减少复制停顿,又绕过了功能检查站的要求。这表明了一个模型,其中检查点作为一种响应机制,可以响应新生的ZGA重塑细胞周期。

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