Single-cell transcriptomic atlas of goat ovarian aging.

IF 6.3 Q1 AGRICULTURE, DAIRY & ANIMAL SCIENCE Journal of Animal Science and Biotechnology Pub Date : 2023-12-06 DOI:10.1186/s40104-023-00948-8
Dejun Xu, Shuaifei Song, Fuguo Wang, Yawen Li, Ziyuan Li, Hui Yao, Yongju Zhao, Zhongquan Zhao
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Abstract

Background: The ovaries are one of the first organs that undergo degenerative changes earlier in the aging process, and ovarian aging is shown by a decrease in the number and quality of oocytes. However, little is known about the molecular mechanisms of female age-related fertility decline in different types of ovarian cells during aging, especially in goats. Therefore, the aim of this study was to reveal the mechanisms driving ovarian aging in goats at single-cell resolution.

Results: For the first time, we surveyed the single-cell transcriptomic landscape of over 27,000 ovarian cells from newborn, young and aging goats, and identified nine ovarian cell types with distinct gene-expression signatures. Functional enrichment analysis showed that ovarian cell types were involved in their own unique biological processes, such as Wnt beta-catenin signalling was enriched in germ cells, whereas ovarian steroidogenesis was enriched in granulosa cells (GCs). Further analysis showed that ovarian aging was linked to GCs-specific changes in the antioxidant system, oxidative phosphorylation, and apoptosis. Subsequently, we identified a series of dynamic genes, such as AMH, CRABP2, THBS1 and TIMP1, which determined the fate of GCs. Additionally, FOXO1, SOX4, and HIF1A were identified as significant regulons that instructed the differentiation of GCs in a distinct manner during ovarian aging.

Conclusions: This study revealed a comprehensive aging-associated transcriptomic atlas characterizing the cell type-specific mechanisms during ovarian aging at the single-cell level and offers new diagnostic biomarkers and potential therapeutic targets for age-related goat ovarian diseases.

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山羊卵巢衰老的单细胞转录组图谱
背景:卵巢是衰老过程中最早发生退行性变化的器官之一,卵巢衰老表现为卵母细胞数量和质量的下降。然而,人们对衰老过程中不同类型卵巢细胞中与雌性年龄相关的生育能力下降的分子机制知之甚少,特别是在山羊中。因此,本研究旨在以单细胞分辨率揭示驱动山羊卵巢衰老的机制:结果:我们首次调查了来自新生山羊、年轻山羊和衰老山羊的 27,000 多个卵巢细胞的单细胞转录组图谱,发现了九种具有不同基因表达特征的卵巢细胞类型。功能富集分析表明,卵巢细胞类型参与了各自独特的生物学过程,例如生殖细胞富集了Wnt beta-catenin信号,而颗粒细胞(GCs)富集了卵巢类固醇生成。进一步的分析表明,卵巢衰老与颗粒细胞在抗氧化系统、氧化磷酸化和细胞凋亡方面的特异性变化有关。随后,我们发现了一系列决定 GCs 命运的动态基因,如 AMH、CRABP2、THBS1 和 TIMP1。此外,我们还发现FOXO1、SOX4和HIF1A是卵巢衰老过程中以不同方式指导GCs分化的重要调控因子:这项研究揭示了一个全面的衰老相关转录组图谱,在单细胞水平上描述了卵巢衰老过程中细胞类型特异性机制的特征,为与年龄相关的山羊卵巢疾病提供了新的诊断生物标志物和潜在的治疗靶点。
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来源期刊
CiteScore
10.30
自引率
0.00%
发文量
822
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