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猪卵母细胞体外成熟过程中翻译受到抑制,尽管帽结合蛋白复合物eIF4F的形成增加且4E-BP1发生了超磷酸化。

Suppression of translation during in vitro maturation of pig oocytes despite enhanced formation of cap-binding protein complex eIF4F and 4E-BP1 hyperphosphorylation.

作者信息

Ellederova Zdenka, Kovarova Hana, Melo-Sterza Fabiana, Livingstone Mark, Tomek Wolfgang, Kubelka Michal

机构信息

Institute of Animal Physiology and Genetics, Academy of Sciences of the Czech Republic, Libechov, Czech Republic.

出版信息

Mol Reprod Dev. 2006 Jan;73(1):68-76. doi: 10.1002/mrd.20368.

DOI:10.1002/mrd.20368
PMID:16211600
Abstract

In this study, we document that the overall rate of protein synthesis decreases during in vitro maturation (IVM) of pig oocytes despite enhanced formation of the 5' cap structure eIF4F. Within somatic/interphase cells, formation of the eIF4F protein complex correlates very well with overall rates of protein translation, and the formation of this complex is controlled primarily by the availability of the 5' cap binding protein eIF4E. We show that the eIF4E inhibitory protein, 4E-BP1, becomes phosphorylated during IVM, which results in gradual release of eIF4E from 4E-BP1, as documented by immunoprecipitation analyses. Isoelectric focusing and Western blotting experiments show conclusively that eIF4E becomes gradually phosphorylated with a maximum at metaphase II (M II). The activity of eIF4E and its ability to bind mRNA also increases during oocyte maturation as documented in experiments with m7-methyl GTP-Sepharose, which mimics the cap structure of mRNA. Complementary analysis of flow-through fraction for 4E-BP1, and eIF4G proteins additionally provides evidence for enhanced formation of cap-binding protein complex eIF4F. Altogether, our results bring new insights to the regulation of translation initiation during meiotic division, and more specifically clarify that 4E-BP1 hyper-phosphorylation is not the cause of the observed suppression of overall translation rates.

摘要

在本研究中,我们记录到,尽管猪卵母细胞体外成熟(IVM)过程中5'帽结构eIF4F的形成有所增强,但蛋白质合成的总体速率却下降了。在体细胞/间期细胞中,eIF4F蛋白复合物的形成与蛋白质翻译的总体速率密切相关,并且该复合物的形成主要受5'帽结合蛋白eIF4E可用性的控制。我们发现,eIF4E抑制蛋白4E-BP1在IVM过程中发生磷酸化,免疫沉淀分析表明,这导致eIF4E从4E-BP1中逐渐释放。等电聚焦和蛋白质印迹实验确凿地表明,eIF4E逐渐发生磷酸化,在中期II(M II)达到最大值。如用模拟mRNA帽结构的m7-甲基GTP-琼脂糖进行的实验所示,eIF4E的活性及其结合mRNA的能力在卵母细胞成熟过程中也会增加。对4E-BP1和eIF4G蛋白的流通部分进行的补充分析进一步证明了帽结合蛋白复合物eIF4F的形成增强。总之,我们的结果为减数分裂期间翻译起始的调控带来了新的见解,更具体地阐明了4E-BP1的过度磷酸化并非观察到的总体翻译速率抑制的原因。

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