The oocyte microenvironment is altered in adolescents compared to oocyte donors.

IF 8.3 Q1 OBSTETRICS & GYNECOLOGY Human reproduction open Pub Date : 2024-08-06 eCollection Date: 2024-01-01 DOI:10.1093/hropen/hoae047
Dilan Gokyer, Sophia Akinboro, Luhan T Zhou, Anna Kleinhans, Monica M Laronda, Francesca E Duncan, Joan K Riley, Kara N Goldman, Elnur Babayev
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Reproductive juvenescence in mammals is associated with suboptimal oocyte quality.</p><p><strong>Study design size duration: </strong>This was a prospective cohort study. Adolescents (10-19 years old, n = 23) and oocyte donors (22-30 years old, n = 31) undergoing ovarian stimulation and oocyte retrieval at a single center between 1 November 2020 and 1 May 2023 were enrolled in this study.</p><p><strong>Participants/materials setting methods: </strong>Patient demographics, ovarian stimulation, and oocyte retrieval outcomes were collected for all participants. The transcriptome of CCs associated with mature oocytes was compared between adolescents (10-19 years old, n = 19) and oocyte donors (22-30 years old, n = 19) using bulk RNA-sequencing. FF cytokine profiles (10-19 years old, n = 18 vs 25-30 years old, n = 16) were compared using cytokine arrays.</p><p><strong>Main results and the role of chance: </strong>RNA-seq analysis revealed 581 differentially expressed genes in CCs of adolescents relative to oocyte donors, with 361 genes downregulated and 220 upregulated. Genes enriched in pathways involved in cell cycle and cell division (e.g. GO: 1903047, <i>P</i> = 3.5 × 10<sup>-43</sup>; GO: 0051983, <i>P</i> = 4.1 × 10<sup>-30</sup>; GO: 0000281, <i>P</i> = 7.7 × 10<sup>-15</sup>; GO: 0044839, <i>P</i> = 5.3 × 10<sup>-13</sup>) were significantly downregulated, while genes enriched in several pathways involved in cellular and vesicle organization (e.g. GO: 0010256, <i>P</i> = 1.2 × 10<sup>-8</sup>; GO: 0051129, <i>P</i> = 6.8 × 10<sup>-7</sup>; GO: 0016050, <i>P</i> = 7.4 × 10<sup>-7</sup>; GO: 0051640, <i>P</i> = 8.1 × 10<sup>-7</sup>) were upregulated in CCs of adolescents compared to oocyte donors. The levels of nine cytokines were significantly increased in FF of adolescents compared to oocyte donors: IL-1 alpha (2-fold), IL-1 beta (1.7-fold), I-309 (2-fold), IL-15 (1.6-fold), TARC (1.9-fold), TPO (2.1-fold), IGFBP-4 (2-fold), IL-12-p40 (1.7-fold), and ENA-78 (1.4-fold). Interestingly, seven of these cytokines have known pro-inflammatory roles. Importantly, neither the CC transcriptomes nor FF cytokine profiles were different in adolescents with or without cancer.</p><p><strong>Large scale data: </strong>Original high-throughput sequencing data have been deposited in Gene Expression Omnibus (GEO) database with the accession number GSE265995.</p><p><strong>Limitations reasons for caution: </strong>This study aims to gain insights into the associated gamete quality by studying the immediate oocyte microenvironment. 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引用次数: 0

Abstract

Study question: Do the molecular signatures of cumulus cells (CCs) and follicular fluid (FF) of adolescents undergoing fertility preservation differ from that of oocyte donors?

Summary answer: The microenvironment immediately surrounding the oocyte, including the CCs and FF, is altered in adolescents undergoing fertility preservation compared to oocyte donors.

What is known already: Adolescents experience a period of subfecundity following menarche. Recent evidence suggests that this may be at least partially due to increased oocyte aneuploidy. Reproductive juvenescence in mammals is associated with suboptimal oocyte quality.

Study design size duration: This was a prospective cohort study. Adolescents (10-19 years old, n = 23) and oocyte donors (22-30 years old, n = 31) undergoing ovarian stimulation and oocyte retrieval at a single center between 1 November 2020 and 1 May 2023 were enrolled in this study.

Participants/materials setting methods: Patient demographics, ovarian stimulation, and oocyte retrieval outcomes were collected for all participants. The transcriptome of CCs associated with mature oocytes was compared between adolescents (10-19 years old, n = 19) and oocyte donors (22-30 years old, n = 19) using bulk RNA-sequencing. FF cytokine profiles (10-19 years old, n = 18 vs 25-30 years old, n = 16) were compared using cytokine arrays.

Main results and the role of chance: RNA-seq analysis revealed 581 differentially expressed genes in CCs of adolescents relative to oocyte donors, with 361 genes downregulated and 220 upregulated. Genes enriched in pathways involved in cell cycle and cell division (e.g. GO: 1903047, P = 3.5 × 10-43; GO: 0051983, P = 4.1 × 10-30; GO: 0000281, P = 7.7 × 10-15; GO: 0044839, P = 5.3 × 10-13) were significantly downregulated, while genes enriched in several pathways involved in cellular and vesicle organization (e.g. GO: 0010256, P = 1.2 × 10-8; GO: 0051129, P = 6.8 × 10-7; GO: 0016050, P = 7.4 × 10-7; GO: 0051640, P = 8.1 × 10-7) were upregulated in CCs of adolescents compared to oocyte donors. The levels of nine cytokines were significantly increased in FF of adolescents compared to oocyte donors: IL-1 alpha (2-fold), IL-1 beta (1.7-fold), I-309 (2-fold), IL-15 (1.6-fold), TARC (1.9-fold), TPO (2.1-fold), IGFBP-4 (2-fold), IL-12-p40 (1.7-fold), and ENA-78 (1.4-fold). Interestingly, seven of these cytokines have known pro-inflammatory roles. Importantly, neither the CC transcriptomes nor FF cytokine profiles were different in adolescents with or without cancer.

Large scale data: Original high-throughput sequencing data have been deposited in Gene Expression Omnibus (GEO) database with the accession number GSE265995.

Limitations reasons for caution: This study aims to gain insights into the associated gamete quality by studying the immediate oocyte microenvironment. The direct study of oocytes is more challenging due to sample scarcity, as they are cryopreserved for future use, but would provide a more accurate assessment of oocyte reproductive potential.

Wider implications of the findings: Our findings have implications for the adolescent fertility preservation cycles. Understanding the expected quality of cryopreserved eggs in this age group will lead to better counseling of these patients about their reproductive potential and may help to determine the number of eggs that is recommended to be banked to achieve a reasonable chance of future live birth(s).

Study funding/competing interests: This project was supported by Friends of Prentice organization SP0061324 (M.M.L. and E.B.), Gesualdo Family Foundation (Research Scholar: M.M.L.), and NIH/NICHD K12 HD050121 (E.B.). The authors have declared that no conflict of interest exists.

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与卵母细胞捐献者相比,青少年的卵母细胞微环境发生了改变。
研究问题:接受生育力保存的青少年的积液细胞(CCs)和卵泡液(FF)的分子特征与卵母细胞捐献者的分子特征是否不同?与卵母细胞捐献者相比,接受生育力保存的青少年卵母细胞周围的微环境(包括CCs和FF)发生了改变:已知情况:青少年在月经初潮后会经历一段亚生殖期。最近的证据表明,这可能至少部分是由于卵母细胞非整倍体增加所致。哺乳动物的生殖青春期与卵母细胞质量不达标有关:这是一项前瞻性队列研究。2020年11月1日至2023年5月1日期间,青少年(10-19岁,n = 23)和卵母细胞捐献者(22-30岁,n = 31)在一个中心接受卵巢刺激和卵母细胞提取:收集了所有参与者的患者人口统计学特征、卵巢刺激和卵母细胞获取结果。使用批量 RNA 测序法比较了青少年(10-19 岁,n = 19)和卵母细胞捐献者(22-30 岁,n = 19)与成熟卵母细胞相关的 CC 的转录组。使用细胞因子阵列比较了FF细胞因子谱(10-19岁,n = 18 vs 25-30岁,n = 16):RNA-seq分析显示,相对于卵细胞捐献者,青少年CC中有581个基因表达不同,其中361个基因下调,220个基因上调。富集在细胞周期和细胞分裂通路中的基因(如:GO: 1903047,P = 3.5 × 10-43;GO: 0051983,P = 4.1 × 10-30;GO: 0000281,P = 7.7 × 10-15;GO: 0044839,P = 5.3 × 10-13)显著下调,而富集在细胞和囊泡组织通路中的基因(如:GO: 0010256,P = 4.1 × 10-30;GO: 0000281,P = 7.7 × 10-15;GO: 0044839,P = 5.3 × 10-13)显著上调。例如,与卵细胞捐献者相比,青少年 CC 中的 GO:0010256,P = 1.2 × 10-8;GO:0051129,P = 6.8 × 10-7;GO:0016050,P = 7.4 × 10-7;GO:0051640,P = 8.1 × 10-7)基因上调。与卵母细胞捐献者相比,青少年 FF 中的九种细胞因子水平明显升高:IL-1α(2倍)、IL-1β(1.7倍)、I-309(2倍)、IL-15(1.6倍)、TARC(1.9倍)、TPO(2.1倍)、IGFBP-4(2倍)、IL-12-p40(1.7倍)和ENA-78(1.4倍)。有趣的是,这些细胞因子中有 7 种具有已知的促炎作用。重要的是,在患有或未患有癌症的青少年中,CC转录组和FF细胞因子谱均无差异:原始高通量测序数据已存入基因表达总库(GEO)数据库,登录号为 GSE265995:本研究旨在通过研究直接的卵母细胞微环境,深入了解相关配子的质量。由于样本稀缺,直接研究卵母细胞更具挑战性,因为卵母细胞是为将来使用而冷冻保存的,但这样可以更准确地评估卵母细胞的生殖潜力:我们的研究结果对青少年生育力保存周期具有重要意义。了解该年龄组冷冻保存卵子的预期质量将有助于更好地向这些患者提供有关其生殖潜能的咨询,并有助于确定建议储存的卵子数量,以实现未来活产的合理机会:本项目得到了普伦蒂斯之友组织 SP0061324(M.M.L.和 E.B.)、Gesualdo 家庭基金会(研究学者:M.M.L.)和美国国立卫生研究院/美国国立卫生研究院 K12 HD050121(E.B.)的支持。作者声明不存在利益冲突。
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Membrane-bound receptor for advanced glycation end products (RAGE) is a stable biomarker of low-quality sperm. Women may not benefit from repeated frozen embryo transfers: a retrospective analysis of the cumulative live birth rate of 43 972 women. Sperm and leukocyte telomere length are related to sperm quality parameters in healthy men from the Led-Fertyl study. Reply: Emerging evidence of endometrial compaction in predicting ART outcomes. Emerging evidence of endometrial compaction in predicting ART outcomes.
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