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Polo-like kinase 1 对于小鼠胚胎的第一次有丝分裂分裂是必不可少的。

Polo-like kinase 1 is essential for the first mitotic division in the mouse embryo.

机构信息

Institute of Animal Physiology, Slovak Academy of Sciences, Kosice, Slovakia.

出版信息

Mol Reprod Dev. 2013 Jul;80(7):522-34. doi: 10.1002/mrd.22188. Epub 2013 Jun 13.

DOI:10.1002/mrd.22188
PMID:23649868
Abstract

Polo-like kinase 1 (PLK1), a member of the serine/threonine protein kinases family, is involved in multiple steps of mitotic progression. It regulates centrosome maturation, mitotic spindle formation, and cytokinesis. While studied extensively in somatic cells, little is known about PLK1 activities in the mammalian preimplantation embryo. We examined the role of PLK1 in the one-cell mouse embryo. Western blotting showed that the PLK1 protein content increased significantly during the S-phase of the one-cell stage and declined during the first mitotic division. Activation of PLK1 preceded nuclear envelope breakdown (NEBD) in both pronuclei at the entry to first embryo mitosis. Immunofluorescence revealed the presence of phosphorylated, active PLK1 (pThr(210) -PLK1) in both male and female pronuclei, and in the microtubule-organizing centers (MTOCs) shortly before NEBD. During the first mitotic metaphase, pThr(210) -PLK1 accumulated at the spindle poles and was also associated with condensed chromosomes. Inhibition of PLK1 activity with a specific PLK1 inhibitor, BI 2536, at the one-cell stage induced the formation of a bipolar spindle that displayed disordered microtubular arrangements and dislocated, condensed chromosomes. Although such embryos entered mitosis, they did not complete mitosis and arrested at metaphase. Time-lapse recording revealed progressive misalignment of condensed chromosomes during first mitotic metaphase. These data indicate that PLK1 activity is not essential for entry into first mitosis, but is required for the events leading up to metaphase-anaphase transition in the one-cell mouse embryo.

摘要

丝氨酸/苏氨酸蛋白激酶家族的一员 Polo 样激酶 1(PLK1)参与有丝分裂进程的多个步骤。它调节中心体成熟、有丝分裂纺锤体形成和胞质分裂。虽然在体细胞中进行了广泛研究,但对哺乳动物着床前胚胎中 PLK1 的活性知之甚少。我们研究了 PLK1 在单细胞小鼠胚胎中的作用。Western blot 显示,PLK1 蛋白含量在单细胞阶段的 S 期显著增加,并在第一次有丝分裂分裂期间下降。PLK1 的激活先于核膜破裂(NEBD)在进入第一次胚胎有丝分裂的两个原核中。免疫荧光显示,在雄性和雌性原核中,以及在 NEBD 之前不久的微管组织中心(MTOCs)中存在磷酸化的、活性的 PLK1(pThr(210)-PLK1)。在第一次有丝分裂中期,pThr(210)-PLK1 在纺锤体两极积累,并且还与浓缩染色体相关联。在单细胞阶段用特异性 PLK1 抑制剂 BI 2536 抑制 PLK1 活性会诱导形成双极纺锤体,显示出紊乱的微管排列和错位、浓缩的染色体。尽管这些胚胎进入有丝分裂,但它们不能完成有丝分裂并在中期停滞。延时记录显示,在第一次有丝分裂中期,浓缩染色体逐渐错位。这些数据表明,PLK1 活性对于进入第一次有丝分裂不是必需的,但对于单细胞小鼠胚胎中从中期到后期的过渡所需的事件是必需的。

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