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首页> 外文期刊>Molecular and Cellular Biology >Mouse emi1 Has an Essential Function in Mitotic Progression during Early Embryogenesis
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Mouse emi1 Has an Essential Function in Mitotic Progression during Early Embryogenesis

机译:小鼠emi1在早期胚胎发生过程中的有丝分裂进程中具有基本功能。

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摘要

For successful mitotic entry and spindle assembly, mitosis-promoting factors are activated at the G2/M transition stage, followed by stimulation of the anaphase-promoting complex (APC), an E3 ubiquitin ligase, to direct the ordered destruction of several critical mitotic regulators. Given that inhibition of APC activity is important for preventing premature or improper ubiquitination and destruction of substrates, several modulators and their regulation mechanisms have been studied. Emi1, an early mitotic inhibitor, is one of these regulatory factors. Here we show, by analyzing Emi1-deficient embryos, that Emi1 is essential for precise mitotic progression during early embryogenesis. Emi1?/? embryos were found to be lethal due to a defect in preimplantation development. Cell proliferation appeared to be normal, but mitotic progression was severely defective during embryonic cleavage. Moreover, multipolar spindles and misaligned chromosomes were frequently observed in Emi1 mutant cells, possibly due to premature APC activation. Our results collectively suggest that the late prophase checkpoint function of Emi1 is essential for accurate mitotic progression and embryonic viability.
机译:对于成功的有丝分裂进入和纺锤体组装,有丝分裂促进因子在G 2 / M过渡阶段被激活,然后刺激后期促进复合体(APC)(一种E3泛素连接酶)来指导有序破坏了几个关键的有丝分裂调节剂。鉴于抑制APC活性对于防止过早或不适当的泛素化和底物破坏很重要,因此已经研究了几种调节剂及其调节机制。早期的有丝分裂抑制剂Emi1是这些调节因子之一。在这里,我们通过分析Emi1缺陷型胚胎显示,Emi1对于早期胚胎发生过程中的精确有丝分裂进程至关重要。发现Emi1 ?/?胚胎由于植入前发育的缺陷而具有致命性。细胞增殖似乎是正常的,但是在卵裂过程中,有丝分裂进程严重缺陷。此外,在Emi1突变细胞中经常观察到多极纺锤体和染色体错位,这可能是由于APC过早活化所致。我们的结果共同表明,Emi1的晚期前期检查点功能对于准确的有丝分裂进程和胚胎生存能力至关重要。

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