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Differential DNA methylation patterns of polycystic ovarian syndrome in whole blood of Chinese women

机译:中国女性全血多囊卵巢综合征的DNA差异甲基化模式

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摘要

As a universally common endocrinopathy in women of reproductive age, the polycystic ovarian syndrome is characterized by composite clinical phenotypes reflecting the contributions of reproductive impact of ovarian dysfunction and metabolic abnormalities with widely varying symptoms resulting from interference of the genome with the environment through integrative biological mechanisms including epigenetics. We have performed a genome-wide DNA methylation analysis on polycystic ovarian syndrome and identified a substantial number of genomic sites differentially methylated in the whole blood of PCOS patients and healthy controls (52 sites, false discovery rate < 0.05 and corresponding p value < 5.68e–06), highly consistently replicating biological pathways extensively implicated in immunity and immunity-related inflammatory disorders (false discovery rate < 0.05) that were reportedly regulated in the DNA methylome from ovarian tissue under PCOS condition. Most importantly, our genome-wide profiling focusing on PCOS patients revealed a large number of DNA methylation sites and their enriched functional pathways significantly associated with diverse clinical features (levels of prolactin, estradiol, progesterone and menstrual cycle) that could serve as novel molecular basis of the clinical heterogeneity observed in PCOS women.
机译:作为育龄妇女普遍存在的内分泌病,多囊卵巢综合征的特征是复合临床表型,反映了卵巢功能障碍和代谢异常的生殖影响的贡献,其症状因基因组通过综合生物学机制对环境的干扰而引起广泛变化包括表观遗传学。我们已经对多囊卵巢综合征进行了全基因组DNA甲基化分析,并鉴定了PCOS患者和健康对照者全血中大量甲基化差异化的基因组位点(52个位点,错误发现率<0.05,相应的p值<5.68e –06),高度一致地复制生物学途径,广泛参与免疫和与免疫相关的炎症性疾病(错误发现率<0.05),据报道在PCOS条件下卵巢组织DNA甲基基因组中存在这种调控。最重要的是,我们针对PCOS患者的全基因组分布图揭示了大量DNA甲基化位点及其丰富的功能途径,这些途径与多种临床特征(催乳素,雌二醇,孕酮和月经周期的水平)显着相关,可以作为新的分子基础在PCOS妇女中观察到的临床异质性。

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