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卵母细胞成熟过程中的蛋白质去泛素化会影响受精过程中的精子功能、多精受精防御和胚胎发育。

Protein deubiquitination during oocyte maturation influences sperm function during fertilisation, antipolyspermy defense and embryo development.

作者信息

Yi Young-Joo, Sutovsky Miriam, Song Won-Hee, Sutovsky Peter

机构信息

Division of Animal Sciences, University of Missouri, S141 ASRC, 920 East Campus Drive, Columbia, MO65211-5300, USA.

出版信息

Reprod Fertil Dev. 2015 Nov;27(8):1154-67. doi: 10.1071/RD14012.

DOI:10.1071/RD14012
PMID:24848520
Abstract

Ubiquitination is a covalent post-translational modification of proteins by the chaperone protein ubiquitin. Upon docking to the 26S proteasome, ubiquitin is released from the substrate protein by deubiquitinating enzymes (DUBs). We hypothesised that specific inhibitors of two closely related oocyte DUBs, namely inhibitors of the ubiquitin C-terminal hydrolases (UCH) UCHL1 (L1 inhibitor) and UCHL3 (L3 inhibitor), would alter porcine oocyte maturation and influence sperm function and embryo development. Aberrant cortical granule (CG) migration and meiotic spindle defects were observed in oocytes matured with the L1 or L3 inhibitor. Embryo development was delayed or blocked in oocytes matured with the general DUB inhibitor PR-619. Aggresomes, the cellular stress-inducible aggregates of ubiquitinated proteins, formed in oocytes matured with L1 inhibitor or PR-619, a likely consequence of impaired protein turnover. Proteomic analysis identified the major vault protein (MVP) as the most prominent protein accumulated in oocytes matured with PR-619, suggesting that the inhibition of deubiquitination altered the turnover of MVP. The mitophagy/autophagy of sperm-contributed mitochondria inside the fertilised oocytes was hindered by DUB inhibitors. It is concluded that DUB inhibitors alter porcine oocyte maturation, fertilisation and preimplantation embryo development. By regulating the turnover of oocyte proteins and mono-ubiquitin regeneration, the DUBs may promote the acquisition of developmental competence during oocyte maturation.

摘要

泛素化是伴侣蛋白泛素对蛋白质进行的共价翻译后修饰。与26S蛋白酶体对接后,泛素通过去泛素化酶(DUBs)从底物蛋白上释放。我们推测,两种密切相关的卵母细胞DUBs的特异性抑制剂,即泛素C末端水解酶(UCH)UCHL1的抑制剂(L1抑制剂)和UCHL3的抑制剂(L3抑制剂),会改变猪卵母细胞的成熟,并影响精子功能和胚胎发育。在用L1或L3抑制剂成熟的卵母细胞中观察到异常的皮质颗粒(CG)迁移和减数分裂纺锤体缺陷。在用通用DUB抑制剂PR - 619成熟的卵母细胞中,胚胎发育延迟或受阻。在用L1抑制剂或PR - 619成熟的卵母细胞中形成了聚集体,即泛素化蛋白的细胞应激诱导聚集体,这可能是蛋白质周转受损的结果。蛋白质组学分析确定主要穹窿蛋白(MVP)是在用PR - 619成熟的卵母细胞中积累最显著的蛋白质,这表明去泛素化的抑制改变了MVP的周转。受精卵母细胞内精子贡献的线粒体的线粒体自噬/自噬受到DUB抑制剂的阻碍。结论是,DUB抑制剂改变猪卵母细胞的成熟、受精和植入前胚胎发育。通过调节卵母细胞蛋白质的周转和单泛素再生,DUBs可能促进卵母细胞成熟过程中发育能力的获得。

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