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卵母细胞和卵丘细胞的代谢协同依赖:对决定卵母细胞发育能力的重要作用。

Metabolic co-dependence of the oocyte and cumulus cells: essential role in determining oocyte developmental competence.

机构信息

School of Women's and Children's Health, Fertility & Research Centre, University of New South Wales Sydney, Sydney, NSW, Australia.

Robinson Research Institute, Adelaide Medical School, The University of Adelaide, Adelaide, SA, Australia.

出版信息

Hum Reprod Update. 2021 Jan 4;27(1):27-47. doi: 10.1093/humupd/dmaa043.

Abstract

BACKGROUND

Within the antral follicle, the oocyte is reliant on metabolic support from its surrounding somatic cells. Metabolism plays a critical role in oocyte developmental competence (oocyte quality). In the last decade, there has been significant progress in understanding the metabolism of the cumulus-oocyte complex (COC) during its final stages of growth and maturation in the follicle. Certain metabolic conditions (e.g. obesity) or ART (e.g. IVM) perturb COC metabolism, providing insights into metabolic regulation of oocyte quality.

OBJECTIVE AND RATIONALE

This review provides an update on the progress made in our understanding of COC metabolism, and the metabolic conditions that influence both meiotic and developmental competence of the oocyte.

SEARCH METHODS

The PubMed database was used to search for peer-reviewed original and review articles. Searches were performed adopting the main terms 'oocyte metabolism', 'cumulus cell metabolism', 'oocyte maturation', 'oocyte mitochondria', 'oocyte metabolism', 'oocyte developmental competence' and 'oocyte IVM'.

OUTCOMES

Metabolism is a major determinant of oocyte quality. Glucose is an essential requirement for both meiotic and cytoplasmic maturation of the COC. Glucose is the driver of cumulus cell metabolism and is essential for energy production, extracellular matrix formation and supply of pyruvate to the oocyte for ATP production. Mitochondria are the primary source of ATP production within the oocyte. Recent advances in real-time live cell imaging reveal dynamic fluctuations in ATP demand throughout oocyte maturation. Cumulus cells have been shown to play a central role in maintaining adequate oocyte ATP levels by providing metabolic support through gap junctional communication. New insights have highlighted the importance of oocyte lipid metabolism for oocyte oxidative phosphorylation for ATP production, meiotic progression and developmental competence. Within the last decade, several new strategies for improving the developmental competence of oocytes undergoing IVM have emerged, including modulation of cyclic nucleotides, the addition of precursors for the antioxidant glutathione or endogenous maturation mediators such as epidermal growth factor-like peptides and growth differentiation factor 9/bone morphogenetic protein 15. These IVM additives positively alter COC metabolic endpoints commonly associated with oocyte competence. There remain significant challenges in the study of COC metabolism. Owing to the paucity in non-invasive or in situ techniques to assess metabolism, most work to date has used in vitro or ex vivo models. Additionally, the difficulty of measuring oocyte and cumulus cell metabolism separately while still in a complex has led to the frequent use of denuded oocytes, the results from which should be interpreted with caution since the oocyte and cumulus cell compartments are metabolically interdependent, and oocytes do not naturally exist in a naked state until after fertilization. There are emerging tools, including live fluorescence imaging and photonics probes, which may provide ways to measure the dynamic nature of metabolism in a single oocyte, potentially while in situ.

WIDER IMPLICATIONS

There is an association between oocyte metabolism and oocyte developmental competence. Advancing our understanding of basic cellular and biochemical mechanisms regulating oocyte metabolism may identify new avenues to augment oocyte quality and assess developmental potential in assisted reproduction.

摘要

背景

在卵泡中,卵母细胞依赖于其周围体细胞的代谢支持。代谢在卵母细胞的发育能力(卵母细胞质量)中起着至关重要的作用。在过去的十年中,人们对卵丘-卵母细胞复合物(COC)在卵泡中生长和成熟的最后阶段的代谢有了重要的认识。某些代谢条件(如肥胖)或辅助生殖技术(如 IVM)会扰乱 COC 代谢,为卵母细胞质量的代谢调控提供了见解。

目的和理由

本文综述了我们对 COC 代谢的理解进展,以及影响卵母细胞减数分裂和发育能力的代谢条件。

检索方法

使用 PubMed 数据库搜索同行评审的原始和综述文章。采用“卵母细胞代谢”、“卵丘细胞代谢”、“卵母细胞成熟”、“卵母细胞线粒体”、“卵母细胞代谢”、“卵母细胞发育能力”和“卵母细胞 IVM”等主要术语进行搜索。

结果

代谢是卵母细胞质量的主要决定因素。葡萄糖是 COC 减数分裂和细胞质成熟所必需的。葡萄糖是卵丘细胞代谢的驱动力,对能量产生、细胞外基质形成和丙酮酸供应给卵母细胞以产生 ATP 至关重要。线粒体是卵母细胞中 ATP 产生的主要来源。实时活细胞成像的最新进展揭示了卵母细胞成熟过程中 ATP 需求的动态波动。已经表明,卵丘细胞通过缝隙连接通讯提供代谢支持,在维持足够的卵母细胞 ATP 水平方面发挥着核心作用。新的研究结果强调了卵母细胞脂质代谢对卵母细胞氧化磷酸化产生 ATP、减数分裂进程和发育能力的重要性。在过去的十年中,出现了几种提高 IVM 卵母细胞发育能力的新策略,包括调节环核苷酸、添加抗氧化谷胱甘肽的前体或内源性成熟介质,如表皮生长因子样肽和生长分化因子 9/骨形态发生蛋白 15。这些 IVM 添加物可积极改变与卵母细胞能力相关的 COC 代谢终点。在 COC 代谢研究中仍然存在重大挑战。由于缺乏非侵入性或原位技术来评估代谢,迄今为止大多数工作都使用了体外或离体模型。此外,在复杂的情况下,单独测量卵母细胞和卵丘细胞代谢的难度导致了经常使用去卵丘卵母细胞,由于卵母细胞和卵丘细胞之间存在代谢上的相互依存关系,并且卵母细胞在受精后才自然处于裸露状态,因此应谨慎解释去卵丘卵母细胞的结果。目前有一些新兴工具,包括实时荧光成像和光子探针,可能为在单个卵母细胞中测量代谢的动态特性提供方法,可能在原位进行。

意义

卵母细胞代谢与卵母细胞的发育能力有关。深入了解调节卵母细胞代谢的基本细胞和生化机制,可能为提高卵母细胞质量和评估辅助生殖中的发育潜力提供新的途径。

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