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Modifications of human growth differentiation factor 9 to improve the generation of embryos from low competence oocytes

机译:修饰人类生长分化因子9以改善低能力卵母细胞的胚胎生成

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摘要

Growth differentiation factor 9 (GDF9) is an oocyte-derived growth factor that plays a critical role in ovarian folliculogenesis and oocyte developmental competence, and belongs to the transforming growth factor-β (TGF-β) family of proteins. Recombinant human GDF9 (hGDF9) is secreted in a latent form, which in the case of the fully processed protein, has the pro-region non-covalently associated with the mature region. In this study we investigated a number of amino acid residues in the mature region of hGDF9 which are different from the corresponding residues in the mouse protein, which is not latent. We designed, expressed and purified four forms of chimeric hGDF9 (M1-M4) which we found to be active in a granulosa cell bioassay. Utilizing a porcine in vitro maturation (IVM) model with inherent low developmental competence (yielding 10-20 blastocysts) we tested the ability of the chimeric hGDF9 proteins to improve oocyte maturation and developmental competence. Interestingly, one of the chimeric proteins, M3, was able to significantly increase the level of embryo production utilizing such low competence oocytes. Our molecular modelling studies suggest that in the case of hGDF9 the Gly(391)Arg mutation likely increases receptor binding affinity thereby creating an active protein for granulosa cells in vitro. However, for an improvement in oocyte developmental competence a second mutation (Ser(412)Pro), which potentially decreases affinity of the mature region for the pro-region, is also required.
机译:生长分化因子9(GDF9)是卵母细胞衍生的生长因子,在卵巢卵泡形成和卵母细胞发育能力中起关键作用,属于蛋白质转化生长因子β(TGF-β)家族。重组人GDF9(hGDF9)以潜在形式分泌,在完全加工的蛋白质中,该潜在形式的前区与成熟区非共价结合。在这项研究中,我们研究了hGDF9成熟区域中的许多氨基酸残基,这些残基与小鼠蛋白质中的相应残基不同,这不是潜在的。我们设计,表达和纯化了四种形式的嵌合hGDF9(M1-M4),我们发现它们在颗粒细胞生物测定中具有活性。利用具有固有的低发育能力(产生10-20个胚泡)的猪体外成熟(IVM)模型,我们测试了嵌合hGDF9蛋白改善卵母细胞成熟和发育能力的能力。有趣的是,利用这种低能力的卵母细胞,一种嵌合蛋白M3能够显着提高胚胎的产生水平。我们的分子模型研究表明,在hGDF9的情况下,Gly(391)Arg突变可能会增加受体结合亲和力,从而为体外的颗粒细胞创建活性蛋白。但是,为了改善卵母细胞的发育能力,还需要第二种突变(Ser(412)Pro),这种突变可能会降低成熟区域对原核区域的亲和力。

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