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通过对一种刺胞动物的研究揭示了后生动物卵母细胞成熟过程中Mos的保守功能。

Conserved functions for Mos in eumetazoan oocyte maturation revealed by studies in a cnidarian.

作者信息

Amiel Aldine, Leclère Lucas, Robert Lucie, Chevalier Sandra, Houliston Evelyn

机构信息

Université Pierre et Marie Curie, Centre National de la Recherche, Villefranche-sur-mer, France.

出版信息

Curr Biol. 2009 Feb 24;19(4):305-11. doi: 10.1016/j.cub.2008.12.054.

Abstract

The kinase Mos, which activates intracellularly the MAP kinase pathway, is a key regulator of animal oocyte meiotic maturation. In vertebrate and echinoderm models, Mos RNA translation upon oocyte hormonal stimulation mediates "cytostatic" arrest of the egg after meiosis, as well as diverse earlier events [1-5]. Our phylogenetic survey has revealed that MOS genes are conserved in cnidarians and ctenophores, but not found outside the metazoa or in sponges. We demonstrated MAP kinase-mediated cytostatic activity for Mos orthologs from Pleurobrachia (ctenophore) and Clytia (cnidarian) by RNA injection into Xenopus blastomeres. Analyses of endogenous Mos in Clytia with morpholino antisense oligonucleotides and pharmacological inhibition demonstrated that Mos/MAP kinase function in postmeiotic arrest is conserved. They also revealed additional roles in spindle formation and positioning, strongly reminiscent of observations in starfish, mouse, and Xenopus. Unusually, cnidarians were found to possess multiple Mos paralogs. In Clytia, one of two maternally expressed paralogs accounted for the majority MAP kinase activation during maturation, whereas the other may be subject to differential translational regulation and have additional roles. Our findings indicate that Mos appeared early during animal evolution as an oocyte-expressed kinase and functioned ancestrally in regulating core specializations of female meiosis.

摘要

激酶Mos可在细胞内激活丝裂原活化蛋白激酶(MAP激酶)信号通路,是动物卵母细胞减数分裂成熟的关键调节因子。在脊椎动物和棘皮动物模型中,卵母细胞受到激素刺激后,Mos RNA的翻译介导了减数分裂后卵子的“细胞静止”停滞,以及多种早期事件[1-5]。我们的系统发育研究表明,MOS基因在刺胞动物和栉水母中保守存在,但在后生动物之外或海绵动物中未发现。我们通过将来自侧腕水母(栉水母)和海月水母(刺胞动物)的Mos直系同源物RNA注射到非洲爪蟾的卵裂球中,证明了MAP激酶介导的细胞静止活性。用吗啉代反义寡核苷酸和药理学抑制方法对海月水母中的内源性Mos进行分析,结果表明Mos/MAP激酶在减数分裂后停滞中的功能是保守的。这些分析还揭示了其在纺锤体形成和定位中的其他作用,这与在海星、小鼠和非洲爪蟾中的观察结果非常相似。不同寻常的是,发现刺胞动物拥有多个Mos旁系同源物。在海月水母中,两个母源表达的旁系同源物之一在成熟过程中占大部分MAP激酶激活,而另一个可能受到不同的翻译调控并具有其他作用。我们的研究结果表明,Mos在动物进化早期作为一种卵母细胞表达的激酶出现,其在调节雌性减数分裂的核心特化方面具有祖先功能。

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