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AURKB and MAPK involvement in the regulation of the early stages of mouse zygote development

机译:AURKB和MAPK参与小鼠合子发育早期的调控

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Aurora kinases have become a hot topic for research as they have been found to play an important role in various stages of mitotic cell division and to participate in malignant conversions of tumors. The participation of Aurora kinases in the regulation of oocyte meiosis has been recently reported, but their participation in mammalian early embryonic development remained unclear. The object of our study was to establish the spatio-temporal expression pattern of Aurora kinase B (AURKB) in mouse zygotes during the first cleavage, to reveal its functions in the early development of mouse zygotes, and to define the involvement of AURKB in mitogen-activated protein kinase ( MAPK ) signaling. Our results showed that in mouse zygotes AURKB expression increased in G1 phase and peaked in M phase. AURKB protein distribution was found to be in association with nuclei and distributed throughout the cytoplasm in a cell cycle-dependent manner. Functional disruption of AURKB resulted in abnormal division phenotypes or mitotic impairments. U0126, a specific mitogen-activated protein kinase kinase (MEK) inhibitor, caused significantly altered morphologies of early embryos together with a decrease in protein expression and kinase activity of AURKB. Our results indicated that the activity of AURKB was required for regulating multiple stages of mitotic progression in the early development of mouse zygotes and was correlated with the activation of the MAPK pathway .
机译:由于发现极光激酶在有丝分裂细胞分裂的各个阶段均起重要作用并参与肿瘤的恶性转化,因此已成为研究的热点。最近已经报道了Aurora激酶参与卵母细胞减数分裂的调控,但是它们在哺乳动物早期胚胎发育中的参与仍不清楚。我们的研究目的是建立在第一次卵裂期间Aurora激酶B(AURKB)在小鼠受精卵中的时空表达模式,以揭示其在小鼠受精卵早期发育中的功能,并确定AURKB在有丝分裂原中的参与。激活的蛋白激酶(MAPK)信号传导。我们的结果表明,在小鼠受精卵中,AURKB表达在G1期增加,在M期达到高峰。发现AURKB蛋白分布与细胞核相关并以细胞周期依赖性方式分布在整个细胞质中。 AURKB的功能破坏导致异常的分裂表型或有丝分裂受损。 U0126是一种特定的促分裂原活化蛋白激酶激酶(MEK)抑制剂,可导致早期胚胎的形态发生显着变化,同时蛋白表达和AURKB激酶活性也下降。我们的结果表明,在小鼠受精卵的早期发育中,AURKB的活性是调节多阶段有丝分裂进程所需要的,并且与MAPK途径的激活有关。

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