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骨形态发生蛋白 15 在卵巢功能中的基本作用及其在女性生育障碍中的作用。

The fundamental role of bone morphogenetic protein 15 in ovarian function and its involvement in female fertility disorders.

机构信息

Department of Clinical Sciences & Community Health, University of Milan, 20100 Milan, Italy Laboratory of Endocrine & Metabolic Research and Division of Endocrine and Metabolic Diseases, IRCCS Istituto Auxologico Italiano, Piazzale Brescia 20, 20149 Milan, Italy

Department of Clinical Sciences & Community Health, University of Milan, 20100 Milan, Italy.

出版信息

Hum Reprod Update. 2014 Nov-Dec;20(6):869-83. doi: 10.1093/humupd/dmu036. Epub 2014 Jun 30.

Abstract

BACKGROUND

A large number of studies have contributed to understanding the general mechanisms driving ovarian folliculogenesis in humans and show a complex endocrine dialog between the central nervous system, the pituitary and the ovary, integrated by various intraovarian paracrine messages. The role of intraovarian paracrine regulation has acquired more relevance in the recent years owing to the discovery of previously unknown factors, such as the oocyte-derived bone morphogenetic protein (BMP)15.

METHODS

A thorough literature search was carried out in order to summarize what has been reported so far on the role of BMP15, and the BMP15 paralog, growth and differentiation factor 9 (GDF9), in ovarian function and female fertility. Research articles published in English until March 2014 were included.

RESULTS

The biological actions of BMP15 include: (i) the promotion of follicle growth and maturation starting from the primary gonadotrophin-independent phases of folliculogenesis; (ii) the regulation of follicular granulosa cell (GC) sensitivity to FSH action and the determination of ovulation quota; (iii) the prevention of GC apoptosis and (iv) the promotion of oocyte developmental competence. The existence of biologically active heterodimers with GDF9, and/or the synergistic co-operation of BMP15 and GDF9 homodimers are indeed relevant in this context. Experimental disruption of the bmp15 gene in mice resulted in a mild fertility defect limited to females, whereas natural missense mutations in ewes cause variable phenotypes (ranging from hyperprolificacy to complete sterility) depending on a fine gene dosage mechanism also involving GDF9. Strong evidence supports the concept that such a mechanism plays an important role in the regulation of ovulation rate across mammalian and non-mammalian species. Following the discovery of sheep fecundity genes, several research groups have focused on alterations in human BMP15 associated with primary ovarian insufficiency (POI) or polycystic ovary syndrome. Several variants of BMP15 are significantly associated with POI supporting their pathogenic role, but the underlying biological mechanism is still under investigation and of great interest in medicine. BMP15 maps to the Xp locus involved in the determination of the ovarian defect in Turner syndrome and significantly contributes to the determination of ovarian reserve. Pioneering studies in women undergoing controlled ovarian stimulation indicate that BMP15 may represent a marker of ovarian response or oocyte quality.

CONCLUSIONS

BMP15, an oocyte-derived growth and differentiation factor, is a critical regulator of folliculogenesis and GC activities. Variations in BMP15 gene dosage have a relevant influence on ovarian function and can account for several defects of female fertility. The modulation of BMP15 action may have interesting pharmacological perspectives and the analysis of BMP15 may become a useful marker in IVF procedures. Recent outcomes indicate that the close interactions of BMP15/GDF9 have a critical biological impact that should be taken into account in future studies.

摘要

背景

大量的研究有助于理解人类卵巢卵泡发生的一般机制,并展示了中枢神经系统、垂体和卵巢之间的复杂内分泌对话,其中整合了各种卵巢内旁分泌信息。由于发现了以前未知的因素,如卵母细胞衍生的骨形态发生蛋白 15(BMP15),卵巢内旁分泌调节的作用近年来变得更加重要。

方法

我们进行了彻底的文献检索,以总结迄今为止关于 BMP15 和其旁系同源物生长分化因子 9(GDF9)在卵巢功能和女性生育力中的作用的报道。纳入了截至 2014 年 3 月发表的英文研究文章。

结果

BMP15 的生物学作用包括:(i)从卵泡发生的初级促性腺激素非依赖性阶段开始促进卵泡生长和成熟;(ii)调节卵泡颗粒细胞(GC)对 FSH 作用的敏感性并决定排卵数量;(iii)防止 GC 凋亡;(iv)促进卵母细胞发育能力。与 GDF9 形成具有生物活性的异二聚体,和/或 BMP15 和 GDF9 同源二聚体的协同合作,在这种情况下确实很重要。在小鼠中破坏 bmp15 基因会导致轻微的生育缺陷,仅限于雌性,而在绵羊中自然发生的错义突变会导致不同的表型(从多产到完全不育),这取决于精细的基因剂量机制,该机制还涉及 GDF9。强有力的证据支持这样一个概念,即这种机制在调节哺乳动物和非哺乳动物的排卵率方面发挥着重要作用。在发现绵羊生育基因之后,几个研究小组专注于与原发性卵巢功能不全(POI)或多囊卵巢综合征相关的人类 BMP15 改变。几种 BMP15 变体与 POI 显著相关,支持其致病作用,但潜在的生物学机制仍在研究中,在医学上具有很大的意义。BMP15 位于 Xp 基因座上,与 Turner 综合征的卵巢缺陷决定有关,并显著影响卵巢储备。在接受控制性卵巢刺激的妇女中的开创性研究表明,BMP15 可能是卵巢反应或卵母细胞质量的标志物。

结论

BMP15 是一种卵母细胞衍生的生长和分化因子,是卵泡发生和 GC 活性的关键调节剂。BMP15 基因剂量的变化对卵巢功能有重要影响,并可导致女性生育力的多种缺陷。BMP15 作用的调节可能具有有趣的药理学前景,BMP15 的分析可能成为 IVF 程序中的有用标志物。最近的结果表明,BMP15/GDF9 的密切相互作用具有重要的生物学影响,在未来的研究中应予以考虑。

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