Division of Obstetrics and Gynecology, Department of Human Reproduction, University Medical Centre Ljubljana, Ljubljana, Slovenia.
Faculty of Medicine, University of Ljubljana, Ljubljana, Slovenia.
Metab Syndr Relat Disord. 2022 Sep;20(7):384-394. doi: 10.1089/met.2021.0149. Epub 2022 Jul 13.
Obese women with polycystic ovarian syndrome (PCOS) have a reduced rate of spontaneous conception even when their cycles are ovulatory. Endometrial receptivity is an important factor for poor implantation and increased miscarriage rates. Mechanisms in which both pathologies modify the endometrium are not fully clarified. The aim of our study was to compare the endometrial transcriptomic profiles between infertile obese PCOS (O-PCOS) women and infertile normal weight subjects during the window of implantation in ovulatory menstrual cycles. We conducted a prospective transcriptomic analysis of the endometrium using RNA sequencing. In this way, potential endometrial mechanisms leading to the poor reproductive outcome in O-PCOS patients could be characterized. Endometrial samples during days 21-23 of the menstrual cycle were collected from infertile O-PCOS women ( = 11) and normal weight controls ( = 10). Subgroups were defined according to the ovulatory/anovulatory status in the natural cycles, and O-PCOS women were grouped into the O-PCOS ovulatory (O-PCOS-ovul) subgroup. RNA isolation, sequencing with library reparation, and subsequent RNAseq data analysis were performed. Infertile O-PCOS patients had 610 differentially expressed genes (DEGs), after adjustment for multiple comparisons with normal weight infertile controls, related to obesity ( and ), PCOS ( and ), and metabolism ( and ). In the ovulatory subgroup, no DEGs were found, but significant differences in canonical pathways and the upstream regulator were revealed. According to functional and upstream analyses of ovulatory subgroup comparisons, the most important biological processes were related to inflammation (TNFR1 signaling), insulin signaling (insulin receptor signaling and PI3/AKT), fatty acid metabolism (stearate biosynthesis I and palmitate biosynthesis I), and lipotoxicity (unfolded protein response pathway). We demonstrated that endometrial transcription in ovulatory O-PCOS patients is deranged in comparison with the control ovulatory endometrium. The most important pathways of differentiation include metabolism and inflammation. These processes could also represent potential mechanisms for poor embryo implantation, which prevent the development of a successful pregnancy. ClinicalTrials.gov ID: NCT03353948.
患有多囊卵巢综合征(PCOS)的肥胖女性,即使其周期排卵,自然受孕的几率也会降低。子宫内膜容受性是影响着床不良和流产率增加的重要因素。这两种病理改变子宫内膜的机制尚未完全阐明。我们的研究目的是比较排卵性月经周期中不孕肥胖多囊卵巢综合征(O-PCOS)女性和不孕正常体重女性的子宫内膜转录组谱。我们使用 RNA 测序对子宫内膜进行了前瞻性转录组分析。通过这种方式,可以描述导致 O-PCOS 患者生殖结局不良的潜在子宫内膜机制。从不孕 O-PCOS 女性(n=11)和正常体重对照组(n=10)的自然周期中采集月经周期第 21-23 天的子宫内膜样本。根据自然周期的排卵/无排卵状态定义亚组,O-PCOS 女性分为 O-PCOS 排卵(O-PCOS-ovul)亚组。进行 RNA 分离、文库制备和随后的 RNAseq 数据分析。调整与正常体重不孕对照组的多重比较后,O-PCOS 患者有 610 个差异表达基因(DEGs),与肥胖(和)、PCOS(和)和代谢(和)有关。在排卵亚组中,未发现差异表达基因,但揭示了经典途径和上游调节剂的显著差异。根据排卵亚组比较的功能和上游分析,最重要的生物学过程与炎症(TNFR1 信号)、胰岛素信号(胰岛素受体信号和 PI3/AKT)、脂肪酸代谢(硬脂酸生物合成 I 和棕榈酸生物合成 I)和脂毒性(未折叠蛋白反应途径)有关。我们证明,与对照排卵子宫内膜相比,排卵 O-PCOS 患者的子宫内膜转录失调。最重要的分化途径包括代谢和炎症。这些过程也可能代表胚胎着床不良的潜在机制,从而阻止成功妊娠的发展。ClinicalTrials.gov ID:NCT03353948。
