Advanced maternal age is associated with a decline in oocyte quality, which often leads to reproductive failure in humans. However, the mechanisms behind this age-related decline remain unclear. To gain insights into this phenomenon, we applied plexDIA, a multiplexed data-independent acquisition, single-cell mass spectrometry method, to analyze the proteome of oocytes from both young women and women of advanced maternal age. Our findings primarily revealed distinct proteomic profiles between immature fully grown germinal vesicle and mature metaphase II oocytes. Importantly, we further show that a woman's age is associated with changes in her oocyte proteome. Specifically, when compared to oocytes obtained from young women, advanced maternal age oocytes exhibited lower levels of the proteasome and TRiC complex, as well as other key regulators of proteostasis and meiosis. This suggests that aging adversely affects the proteostasis and meiosis networks in human oocytes. The proteins identified in this study hold potential as targets for improving oocyte quality and may guide future studies into the molecular processes underlying oocyte aging.
Single-cell proteomics reveals decreased abundance of proteostasis and meiosis proteins in advanced maternal age oocytes.
单细胞蛋白质组学研究揭示,高龄母亲卵母细胞中蛋白质稳态和减数分裂蛋白的丰度降低
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作者:Galatidou Styliani, Petelski Aleksandra A, Pujol Aïda, Lattes Karinna, Latorraca Lais B, Fair Trudee, Popovic Mina, Vassena Rita, Slavov Nikolai, Barragán Montserrat
| 期刊: | Molecular Human Reproduction | 影响因子: | 3.500 |
| 时间: | 2024 | 起止号: | 2024 Jun 26; 30(7):gaae023 |
| doi: | 10.1093/molehr/gaae023 | 研究方向: | 细胞生物学 |
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