High-throughput mRNA sequencing of stromal cells from endometriomas and endometrium
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High-throughput mRNA sequencing of endometrioma stromal cells identified over 1300 dysregulated genes and highlighted major imbalances in complement regulation compared to eutopic endometrial stromal cells.
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Abstract
Abstract The aetiology of endometriosis is still unclear and to find mechanisms behind the disease development, it is important to study each cell type from endometrium and ectopic lesions independently. The objective of this study was to uncover complete mRNA profiles in uncultured stromal cells from paired samples of endometriomas and eutopic endometrium. High-throughput mRNA sequencing revealed over 1300 dysregulated genes in stromal cells from ectopic lesions, including several novel genes in the context of endometriosis. Functional annotation analysis of differentially expressed genes highlighted pathways related to cell adhesion, extracellular matrix–receptor interaction and complement and coagulation cascade. Most importantly, we found a simultaneous upregulation of complement system components and inhibitors, indicating major imbalances in complement regulation in ectopic stromal cells. We also performed in vitro experiments to evaluate the effect of endometriosis patients’ peritoneal fluid (PF) on complement system gene expression levels, but no significant impact of PF on C3, CD55 and CFH levels was observed. In conclusion, the use of isolated stromal cells enables to determine gene expression levels without the background interference of other cell types. In the future, a new standard design studying all cell types from endometriotic lesions separately should be applied to reveal novel mechanisms behind endometriosis pathogenesis.
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Cited by (25)
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- Complement and coagulation cascade cross-talk in endometriosis and the potential of Janus Kinase inhibitors—a network meta-analysis 2025
- Complement and coagulation cascade cross-talk in endometriosis and the potential of JAK inhibitors – a network meta-analysis 2025
- Endometriosis: Pathogenesis, Diagnosis and Treatment, volume II 2024
- Using a Quantitative High-Throughput Screening Platform to Identify Molecular Targets and Compounds as Repurposing Candidates for Endometriosis 2023
- Análise exploratória do miRNoma de células-tronco mesenquimais isoladas de fluxo menstrual de mulheres com endometriose 2023
- Identification and analysis of novel endometriosis biomarkers via integrative bioinformatics 2022
- Histone H3K4me3 breadth in hypoxia reveals endometrial core functions and stress adaptation linked to endometriosis 2022
- What Do the Transcriptome and Proteome of Menstrual Blood-Derived Mesenchymal Stem Cells Tell Us about Endometriosis? 2022
- The expression pattern of endometrial receptivity genes is desynchronized between endometrium and matched endometriomas 2022
- Transcriptome Profiling of Eutopic and Ectopic Endometrial Stromal Cells in Women with Endometriosis Based on High-Throughput Sequencing 2022
- What do the Transcriptome and Proteome of Menstrual Blood-derived Mesenchymal Stem Cells Tell us about Endometriosis? 2022
- Immunological Basis of the Endometriosis: The Complement System as a Potential Therapeutic Target 2021
- Multi‐omics analysis reveals the interaction between the complement system and the coagulation cascade in the development of endometriosis 2021
- The Inflammatory Feed-Forward Loop Triggered by the Complement Component C3 as a Potential Target in Endometriosis 2021
- MiR‐370‐3p inhibits the development of human endometriosis by downregulating EDN1 expression in endometrial stromal cells 2021
- Complement Component 3 expressed by the endometrial ectopic tissue is involved in the endometriotic lesion formation through mast cell activation 2020
- A relational database to identify differentially expressed genes in the endometrium and endometriosis lesions 2020
- CTHRC1 overexpression promotes ectopic endometrial stromal cell proliferation, migration and invasion via activation of the Wnt/β-catenin pathway 2019
- Endometrial Immune-Inflammatory Gene Signatures in Endometriosis 2019
- Transcriptomic responses to hypoxia in endometrial and decidual stromal cells 2019
- lncRNA/mRNA profiling of endometriosis rat uterine tissues during the implantation window 2019
- Differentially-Expressed miRNAs in Ectopic Stromal Cells Contribute to Endometriosis Development: The Plausible Role of miR-139-5p and miR-375 2018
- DNA methylation alterations—potential cause of endometriosis pathogenesis or a reflection of tissue heterogeneity?† 2018
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