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鉴定卵巢储备功能降低女性的独特表观遗传特征。

Identification of a unique epigenetic profile in women with diminished ovarian reserve.

机构信息

Department of Obstetrics and Gynaecology, Department of Reproductive Medicine, Hospital Herlev, Copenhagen University, Copenhagen, Denmark; DNRF Center for Chromosome Stability, Department of Cellular and Molecular Medicine, Faculty of Health and Medical Sciences, University of Copenhagen, Copenhagen, Denmark.

Epigenetics Programme, Babraham Institute, Cambridge, United Kingdom.

出版信息

Fertil Steril. 2021 Mar;115(3):732-741. doi: 10.1016/j.fertnstert.2020.09.009. Epub 2020 Dec 4.

Abstract

OBJECTIVE

To investigate whether epigenetic profiles of mural granulosa cells (MGC) and leukocytes from women with diminished ovarian reserve (DOR) differ from those of women with normal or high ovarian reserve.

DESIGN

Prospectively collected material from a multicenter cohort of women undergoing fertility treatment.

SETTING

Private and university-based facilities for clinical services and research.

PATIENT(S): One hundred and nineteen women of various ages and ovarian reserve status (antimüllerian hormone level) who provided blood samples and MGC.

INTERVENTION(S): None.

MAIN OUTCOME MEASURE(S): Measures of epigenetic aging rates from whole-genome methylation array data: DNA methylation variability, age acceleration, DNA methylation telomere length estimator (DNAmTL), and accumulation of epimutations.

RESULT(S): Comparison of DOR or high ovarian reserve samples to controls (normal ovarian reserve) showed differential methylation variability between DOR and normal samples at 4,199 CpGs in MGC, and 447 between high and normal (false-discovery rate < 0.05). Variable sites in MGC from DOR were enriched in regions marked with the repressive histone modification H3K27me3, and also included genes involved in folliculogenesis, such as insulin growth factor 2 (IGF2) and antimüllerian hormone (AMH). Regardless of ovarian reserve, very few signals were detected in leukocytes, and no overlaps with those in MGC were found. Furthermore, we found a higher number of epimutations in MGC from women with DOR (Kruskal-Wallis test, difference in mean = 3,485).

CONCLUSION(S): The somatic cells of human ovarian follicles have a distinctive epigenetic profile in women with DOR. A high frequency of epimutations suggests premature aging. Ovarian reserve status was not reflected in the leukocyte epigenetic profile.

摘要

目的

研究卵巢储备功能降低(DOR)女性的壁层颗粒细胞(MGC)和白细胞的表观遗传谱是否与正常或高卵巢储备功能的女性不同。

设计

前瞻性收集接受生育治疗的多中心队列女性的材料。

地点

为临床服务和研究提供私人和大学设施的场所。

患者

119 名年龄和卵巢储备状态(抗苗勒管激素水平)不同的女性,她们提供了血液样本和 MGC。

干预措施

无。

主要观察指标

全基因组甲基化阵列数据的表观遗传衰老率测量:DNA 甲基化变异性、年龄加速、DNA 甲基化端粒长度估计器(DNAmTL)和表观遗传突变积累。

结果

与对照组(正常卵巢储备)相比,DOR 或高卵巢储备样本显示 MGC 中 4199 个 CpG 处的 DOR 和正常样本之间的差异甲基化变异性,447 个 CpG 处高和正常样本之间存在差异(错误发现率<0.05)。DOR 中 MGC 的可变位点在具有抑制性组蛋白修饰 H3K27me3 标记的区域中富集,并且还包括与卵泡发生相关的基因,如胰岛素生长因子 2(IGF2)和抗苗勒管激素(AMH)。无论卵巢储备如何,在白细胞中很少检测到信号,并且没有发现与 MGC 中信号的重叠。此外,我们发现 DOR 女性的 MGC 中存在更多的表观遗传突变(Kruskal-Wallis 检验,平均差异=3485)。

结论

人类卵巢卵泡的体细胞在 DOR 女性中具有独特的表观遗传谱。高频率的表观遗传突变提示过早衰老。白细胞的表观遗传特征不能反映卵巢储备状态。

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