Stem cell-conditioned medium improves methylation patterns and quality of caprine preantral follicles.

IF 3.7 3区 生物学 Q1 DEVELOPMENTAL BIOLOGY
Reproduction Pub Date : 2024-08-14 Print Date: 2024-09-01 DOI:10.1530/REP-23-0483
Ana Flávia B Silva, Laritza Ferreira Lima, Renata Patrícia Sousa, Renato Félix Silva, Gustavo Cardoso S Neves, Maria Acelina M Carvalho, Anna Clara A Ferreira, Ariclécio Cunha Oliveira, Benner Geraldo Alves, Ana Paula R Rodrigues, Eduardo Leite Gastal, Vilceu Bordignon, José Ricardo Figueiredo
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引用次数: 0

Abstract

In brief: Conditioned medium from Wharton's jelly mesenchymal stem cells improved tissue and preantral follicle outcomes, preventing adverse effects of oxidative stress, apoptosis, and epigenetic changes.

Abstract: This study investigated the methylation patterns of H3K4me3 and H3K9me3, as well as the mRNA expression of genes encoding the epigenetic regulators KDM1AX1, KDM1AX2, and KDM3A in goat preantral follicles developed in vivo (Uncultured control) or after in vitro culture for 7 days in either the absence (α-MEM+) or presence of conditioned medium (α-MEM+ + CM) from Wharton's jelly mesenchymal stem cells (WJ-MSCs). In the invivo setting, all follicular categories exhibited similar H3K4me3 and H3K9me3 patterns, and transcripts of KDM1AX1, KDM1AX2, and KDM3A were detected in all samples. During in vitro culture, α-MEM+ + CM enhanced several important aspects. It increased the percentage of normal growing follicles, oocyte diameters across all categories, stromal cell density, and the H3K4me3 methylation pattern in preantral follicles. Simultaneously, it decreased the levels of reduced thiols and reactive oxygen species in the spent media, diminished the presence of lipofuscin aggresomes, lowered granulosa cell apoptotic rates, and reduced the H3K9me3 methylation pattern in preantral follicles. In conclusion, the findings from this study provide compelling evidence that supplementing the in vitro culture medium (α-MEM+) with CM from WJ-MSCs has a protective effect on goat preantral follicles. Notably, CM supplementation preserved follicular survival, as evidenced by enhanced follicular and oocyte growth and increased stromal cell density when compared to the standard culture conditions in the α-MEM+ medium. Furthermore, CM reduced oxidative stress and apoptosis and promoted alterations in H3K4me3 and H3K9me3 patterns.

干细胞调节培养基可改善甲基化模式和黄羊前卵泡的质量。
本研究调查了体内发育的山羊前卵泡(未培养对照)或在无α-MEM+或有α-MEM+的条件下体外培养7天后的山羊前卵泡中H3K4me3和H3K9me3的甲基化模式以及编码表观遗传调节因子KDM1AX1、KDM1AX2和KDM3A的基因的mRNA表达、和 KDM3A 的基因表达。在体内环境中,所有卵泡类别都表现出相似的H3K4me3和H3K9me3模式,并且在所有样本中都检测到了KDM1AX1、KDM1AX2和KDM3A的转录本。在体外培养过程中,α-MEM+ + CM增强了几个重要方面。它提高了正常生长卵泡的百分比、各类卵母细胞的直径、基质细胞密度以及前胚叶卵泡的 H3K4me3 甲基化模式。同时,它还降低了废培养基中还原型硫醇和活性氧的水平,减少了脂褐素凝集体的存在,降低了颗粒细胞凋亡率,并减少了前胚乳卵泡中的 H3K9me3 甲基化模式。总之,本研究的结果提供了令人信服的证据,证明在体外培养基(α-MEM+)中补充 WJ-间充质干细胞的 CM 对山羊前胚乳卵泡有保护作用。值得注意的是,与在α-MEM+培养基中的标准培养条件相比,补充CM能提高卵泡和卵母细胞的生长速度,增加基质细胞密度,从而保护卵泡存活。此外,CM 还能减少氧化应激和细胞凋亡,促进 H3K4me3 和 H3K9me3 模式的改变。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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来源期刊
Reproduction
Reproduction 生物-发育生物学
CiteScore
7.40
自引率
2.60%
发文量
199
审稿时长
4-8 weeks
期刊介绍: Reproduction is the official journal of the Society of Reproduction and Fertility (SRF). It was formed in 2001 when the Society merged its two journals, the Journal of Reproduction and Fertility and Reviews of Reproduction. Reproduction publishes original research articles and topical reviews on the subject of reproductive and developmental biology, and reproductive medicine. The journal will consider publication of high-quality meta-analyses; these should be submitted to the research papers category. The journal considers studies in humans and all animal species, and will publish clinical studies if they advance our understanding of the underlying causes and/or mechanisms of disease. Scientific excellence and broad interest to our readership are the most important criteria during the peer review process. The journal publishes articles that make a clear advance in the field, whether of mechanistic, descriptive or technical focus. Articles that substantiate new or controversial reports are welcomed if they are noteworthy and advance the field. Topics include, but are not limited to, reproductive immunology, reproductive toxicology, stem cells, environmental effects on reproductive potential and health (eg obesity), extracellular vesicles, fertility preservation and epigenetic effects on reproductive and developmental processes.
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