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Stromal fibroblasts from perimenopausal endometrium exhibit a different transcriptome than those from the premenopausal endometrium

机译:绝经前子宫内膜的间质成纤维细胞与绝经前子宫内膜的成纤维细胞具有不同的转录组

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摘要

Human endometrium undergoes extensive regeneration on a cyclic basis in premenopausal women and likely occurs through the contribution of stem/progenitor cells. Menopause results in the permanent cessation of menstrual cycles and is preceded by perimenopause, a period of several years in which endocrine and biological changes occur and is a period of risk for endometrial proliferative disorders. The objectives of this study were to identify endometrial mesenchymal stem cells (eMSC) and endometrial stromal fibroblasts (eSF) in endometrium of perimenopausal women and perform expression profile analysis of perimenopausal eMSC and eSF to gain insight into the biology of stem/progenitor and lineage cell populations during the transition to menopause. Endometrial tissue was collected from perimenopausal and premenopausal women (n = 9 each). Microarray analysis was performed on fluorescence-activated cell sorting-isolated eSF and eMSC, and data were validated by quantitative real-time PCR. Principal component analysis showed that cells clustered into three distinct groups in 3-dimensional space: perimenopausal eMSC and premenopausal eMSC clustered together, while perimenopausal eSF and premenopausal eSF formed two discrete clusters separate from eMSC. Hierarchical clustering revealed a branching pattern consistent with principle clustering analysis results, indicating that eMSC from premenopausal and perimenopausal women exhibit similar transcriptomic signatures. Pathway analysis revealed dysregulation of cytoskeleton, proliferation, and survival pathways in perimenopausal vs. premenopausal eSF. These data demonstrate that cell populations have altered gene expression in perimenopausal vs. premenopausal endometrium, and that perimenopausal eSF had altered pathway activation when compared to premenopausal eSF. This study provides insight into aging endometrium with relevance to function in reproductively older women.
机译:绝经前妇女的子宫内膜周期性地进行大量再生,并且可能通过干/祖细胞的贡献而发生。更年期导致月经周期的永久停止,并在更年期之前,这是发生内分泌和生物学变化的几年,是子宫内膜增生性疾病的危险期。这项研究的目的是确定围绝经期妇女子宫内膜的子宫内膜间充质干细胞(eMSC)和子宫内膜基质成纤维细胞(eSF),并进行围绝经期eMSC和eSF的表达谱分析,以深入了解干/祖细胞和沿袭细胞的生物学特性人口向更年期过渡。从绝经前和绝经前妇女(每例n = 9)收集子宫内膜组织。在荧光激活细胞分选分离的eSF和eMSC上进行微阵列分析,并通过实时定量PCR验证数据。主成分分析表明,细胞在3维空间中分为三个不同的组:围绝经期eMSC和围绝经前eMSC聚集在一起,而围绝经期eSF和围绝经前eSF形成两个独立的簇,与eMSC分开。分层聚类揭示了与原理聚类分析结果一致的分支模式,表明来自绝经前和绝经前妇女的eMSC表现出相似的转录组特征。途径分析显示绝经前与绝经前eSF的细胞骨架,增殖和生存途径失调。这些数据表明,绝经前期与绝经前期子宫内膜细胞群体的基因表达发生了改变,与绝经前期eSF相比,绝经前期eSF的通路激活发生了改变。这项研究提供了有关子宫内膜衰老与生殖年长妇女功能有关的见解。

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