High-throughput mRNA sequencing of stromal cells from endometriomas and endometrium
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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Cited by (25)
- Single-cell transcriptome unveils mesenchymal cell diversity in endometriosis 2025
- 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
- Challenges in endometriosis miRNA studies — From tissue heterogeneity to disease specific miRNAs 2017
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