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首页> 外文期刊>The biochemical journal >Natural occurrence and physiological role of a truncated eIF4E in the porcine endometrium during implantation
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Natural occurrence and physiological role of a truncated eIF4E in the porcine endometrium during implantation

机译:猪子宫内膜在植入过程中自然发生的eIF4E截短和生理作用

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pThe present study is the first report providing evidence for a physiological role of a truncated form of the mRNA cap-binding protein eIF4E1 (eukaryotic initiation factor 4E1). Our initial observation was that eIF4E, which mediates the mRNA cap function by recruiting the eIF4F complex (composed of eIF4E, 4G and 4A), occurs in two forms in porcine endometrial tissue in a strictly temporally restricted fashion. The ubiquitous prototypical 25 kDa form of eIF4E was found in ovariectomized and cyclic animals. A new stable 23 kDa variant, however, is predominant during early pregnancy at the time of implantation. Northern blotting, cDNA sequence analysis, iin vitro/i protease assays and MS showed that the 23 kDa form does not belong to a new class of eIF4E proteins. It represents a proteolytically processed variant of eIF4E1, lacking not more than 21 amino acids at the N-terminus. Steroid replacements indicated that progesterone in combination with 17β-oestradiol induced the formation of the 23 kDa eIF4E. Modified cell-free translation systems mimicking the situation in the endometrium revealed that, besides eIF4E, eIF4G was also truncated, but not eIF4A or PABP [poly(A)-binding protein]. The 23 kDa form of eIF4E reduced the repressive function of 4E-BP1 (eIF4E-binding protein 1) and the truncated eIF4G lacked the PABP-binding site. Thus we suggest that the truncated eIF4E provides an alternative regulation mechanism by an altered dynamic of eIF4E/4E-BP1 binding under conditions where 4E-BP1 is hypophosphorylated. Together with the impaired eIF4G–PABP interaction, the modified translational initiation might particularly regulate protein synthesis during conceptus attachment at the time of implantation./p
机译:>本研究是第一个报告,提供了mRNA帽结合蛋白eIF4E1(真核起始因子4E1)的截短形式的生理作用的证据。我们最初的观察结果是,通过募集eIF4F复合体(由eIF4E,4G和4A组成)介导mRNA帽功能的eIF4E以严格的时间限制方式在猪子宫内膜组织中以两种形式出现。在卵巢切除和周期性动物中发现了普遍存​​在的25kDa的eIF4E原型。然而,新的稳定的23kDa变异体在植入初期的怀孕初期占主导地位。 Northern印迹,cDNA序列分析,体外蛋白酶测定和MS表明23kDa形式不属于一类新的eIF4E蛋白。它代表eIF4E1的蛋白水解加工变体,在N端不超过21个氨基酸。类固醇替代表明孕酮与17β-雌二醇组合诱导了23kDa eIF4E的形成。模仿子宫内膜情况的改良的无细胞翻译系统显示,除eIF4E外,eIF4G也被截短,但eIF4A或PABP [poly(A)结合蛋白]未被截短。 eIF4E的23 kDa形式降低了4E-BP1(eIF4E结合蛋白1)的阻遏功能,而截短的eIF4G则缺少PABP结合位点。因此,我们认为,在4E-BP1被磷酸化的条件下,截短的eIF4E通过改变eIF4E / 4E-BP1结合的动力学提供了一种替代的调控机制。与受损的eIF4G-PABP相互作用一起,修饰的翻译起始可能特别在植入时的概念附着过程中调节蛋白质的合成。

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