Department of Pathology & Immunology, Baylor College of Medicine, Houston, TX 77030, USA.
Graduate Program in Molecular & Cellular Biology, Baylor College of Medicine, Houston, TX 77030, USA.
Development. 2019 Dec 2;146(23):dev176701. doi: 10.1242/dev.176701.
The number and quality of oocytes within the ovarian reserve largely determines fertility and reproductive lifespan in mammals. An oocyte-specific transcription factor cascade controls oocyte development, and some of these transcription factors, such as newborn ovary homeobox gene (), are candidate genes for primary ovarian insufficiency in women. Transcription factors are frequently modified by the post-translational modification SUMOylation, but it is not known whether SUMOylation is required for function of the oocyte-specific transcription factors or if SUMOylation is required in oocytes during their development within the ovarian follicle. To test this, the sole E2 SUMO-conjugating enzyme, , was ablated in mouse oocytes beginning in primordial follicles. Loss of oocyte resulted in female infertility with major defects in stability of the primordial follicle pool, ovarian folliculogenesis, ovulation and meiosis. Transcriptomic profiling of ovaries suggests that loss of oocyte caused defects in both oocyte- and granulosa cell-expressed genes, including NOBOX and some of its known target genes. Together, these studies show that SUMOylation is required in the mammalian oocyte during folliculogenesis for both oocyte development and communication with ovarian somatic cells.
卵巢储备中卵母细胞的数量和质量在很大程度上决定了哺乳动物的生育能力和生殖寿命。卵母细胞特异性转录因子级联控制卵母细胞的发育,其中一些转录因子,如新生卵巢同源盒基因 (),是女性原发性卵巢功能不全的候选基因。转录因子经常通过翻译后修饰 SUMOylation 进行修饰,但尚不清楚 SUMOylation 是否是卵母细胞特异性转录因子功能所必需的,或者在卵母细胞在卵巢卵泡内发育过程中是否需要 SUMOylation。为了检验这一点,在原始卵泡中开始敲除小鼠卵母细胞中唯一的 E2 SUMO 连接酶 。卵母细胞中缺失导致雌性不孕,主要缺陷在于原始卵泡库、卵巢卵泡发生、排卵和减数分裂的稳定性。对卵巢的转录组谱分析表明,卵母细胞中缺失导致卵母细胞和颗粒细胞表达的基因均出现缺陷,包括 和其一些已知的靶基因。总之,这些研究表明,SUMOylation 在哺乳动物卵母细胞的卵泡发生过程中对于卵母细胞的发育和与卵巢体细胞的通讯都是必需的。
