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一种改良卵母细胞发育能力的人生长分化因子-9 变体。

A variant of human growth differentiation factor-9 that improves oocyte developmental competence.

机构信息

Biomedicine Discovery Institute, Monash University, Clayton, Victoria, Australia.

Department of Physiology, Monash University, Clayton, Victoria, Australia.

出版信息

J Biol Chem. 2020 Jun 5;295(23):7981-7991. doi: 10.1074/jbc.RA120.013050. Epub 2020 Apr 29.

Abstract

Growth differentiation factor-9 (GDF9) and bone morphogenetic protein-15 (BMP15) are co-expressed exclusively in oocytes throughout most of folliculogenesis and play central roles in controlling ovarian physiology. Although both growth factors exist as homodimers, recent evidence indicates that GDF9 and BMP15 can also heterodimerize to form the potent growth factor cumulin. Within the cumulin complex, BMP15 "activates" latent GDF9, enabling potent signaling in granulosa cells via type I receptors ( activin receptor-like kinase-4/5 (ALK4/5)) and SMAD2/3 transcription factors. In the cumulin heterodimer, two distinct type I receptor interfaces are formed compared with homodimeric GDF9 and BMP15. Previous studies have highlighted the potential of cumulin to improve treatment of female infertility, but, as a noncovalent heterodimer, cumulin is difficult to produce and purify without contaminating GDF9 and BMP15 homodimers. In this study we addressed this challenge by focusing on the cumulin interface formed by the helix of the GDF9 chain and the fingers of the BMP15 chain. We demonstrate that unique BMP15 finger residues at this site (Arg, Gly, His, and Met) enable potent activation of the SMAD2/3 pathway. Incorporating these BMP15 residues into latent GDF9 generated a highly potent growth factor, called hereafter Super-GDF9. Super-GDF9 was >1000-fold more potent than WT human GDF9 and 4-fold more potent than cumulin in SMAD2/3-responsive transcriptional assays in granulosa cells. Our demonstration that Super-GDF9 can effectively promote mouse cumulus cell expansion and improve oocyte quality represents a potential solution to the current challenges of producing and purifying intact cumulin.

摘要

生长分化因子 9(GDF9)和骨形态发生蛋白 15(BMP15)在大多数卵泡发生过程中仅在卵母细胞中共同表达,并在控制卵巢生理中发挥核心作用。尽管这两种生长因子都以同源二聚体的形式存在,但最近的证据表明,GDF9 和 BMP15 也可以异二聚化形成有效的生长因子 cumulin。在 cumulin 复合物中,BMP15“激活”潜伏的 GDF9,通过 I 型受体(激活素受体样激酶 4/5(ALK4/5))和 SMAD2/3 转录因子使颗粒细胞产生有效信号。在 cumulin 异二聚体中,与同源二聚体 GDF9 和 BMP15 相比,形成了两个不同的 I 型受体界面。先前的研究强调了 cumulin 改善女性不孕治疗的潜力,但由于 cumulin 是一种非共价异二聚体,因此在不污染 GDF9 和 BMP15 同源二聚体的情况下,很难生产和纯化。在这项研究中,我们通过专注于 GDF9 链的螺旋和 BMP15 链的手指形成的 cumulin 界面来解决这一挑战。我们证明,该位点处的独特 BMP15 指状残基(Arg、Gly、His 和 Met)能够有效地激活 SMAD2/3 途径。将这些 BMP15 残基整合到潜伏的 GDF9 中,产生了一种非常有效的生长因子,此后称为 Super-GDF9。Super-GDF9 比 WT 人 GDF9 强 1000 倍以上,在颗粒细胞中 SMAD2/3 反应性转录测定中比 cumulin 强 4 倍。我们的研究结果表明,Super-GDF9 可以有效地促进小鼠卵丘细胞的扩张并提高卵母细胞质量,这为当前生产和纯化完整 cumulin 所面临的挑战提供了一种潜在的解决方案。

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