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首页> 外文期刊>Biochimica et biophysica acta. Molecular cell research >Formin mDia1, a downstream molecule of FMNL1, regulates Profilin1 for actin assembly and spindle organization during mouse oocyte meiosis
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Formin mDia1, a downstream molecule of FMNL1, regulates Profilin1 for actin assembly and spindle organization during mouse oocyte meiosis

机译:Formin mDia1,FMNL1的下游分子,在小鼠卵母细胞减数分裂过程中调节Profilin1的肌动蛋白组装和纺锤体组织

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Mammalian diaphanous1 (mDia1) is a homologue of Drosophila diaphanous and belongs to the Forminhomology family of proteins that catalyze actin nucleation and polymerization. Although Formin family proteins, such as Drosophila diaphanous, have been shown to be essential for cytokinesis, whether and how mDia1 functions during meiosis remain uncertain. In this study, we explored possible roles and the signaling pathway involved for mDia1 using a mouse oocyte model. mDia1 depletion reduced polar body extrusion, which may have been due to reduced cortical actin assembly. mDia1 and Profilin1 had similar localization patterns in mouse oocytes and mDia1 knockdown resulted in reduced Profilin1 expression. Depleting FMNL1, another Formin family member, resulted in reduced mDia1 expression, while RhoA inhibition did not alter mDia1 expression, which indicated that there was a FMNL1-mDia1-Profilin1 signaling pathway in mouse oocytes. Additionally, mDia1 knockdown resulted in disrupting oocyte spindle morphology, which was confirmed by aberrant p-MAPK localization. Thus, these results demonstrated indispensable roles for mDia1 in regulating mouse oocyte meiotic maturation through its effects on actin assembly and spindle organization. (C) 2014 Elsevier B.V. All rights reserved.
机译:哺乳动物diaphanous1(mDia1)是Drosophila diaphanous的同系物,属于催化肌动蛋白成核和聚合反应的蛋白质形态学家族。尽管已显示出Formin家族蛋白(如果蝇)对于胞质分裂是必不可少的,但mDia1在减数分裂过程中是否起作用以及如何发挥作用仍不确定。在这项研究中,我们使用小鼠卵母细胞模型探讨了mDia1的可能作用和信号通路。 mDia1耗竭减少了极体挤压,这可能是由于皮质肌动蛋白组装减少所致。 mDia1和Profilin1在小鼠卵母细胞中具有相似的定位模式,而mDia1敲低导致Profilin1表达降低。耗尽另一家Formin家族成员FMNL1,导致mDia1表达降低,而RhoA抑制却没有改变mDia1表达,这表明小鼠卵母细胞中存在FMNL1-mDia1-Profilin1信号通路。另外,mDia1的敲低导致卵母细胞纺锤体形态的破坏,这可通过异常的p-MAPK定位得到证实。因此,这些结果证明mDia1通过对肌动蛋白组装和纺锤体组织的影响在调节小鼠卵母细胞减数分裂成熟中起着不可或缺的作用。 (C)2014 Elsevier B.V.保留所有权利。

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