LINC01140/miR-200c-3p and LINC01550/miR-363-3p networks play pivotal role in orchestrating progression of endometriosis†
article
OA: closed
CC0
AI-generated summary
This study identified LINC01140/miR-200c-3p and LINC01550/miR-363-3p networks upregulated in endometriosis, promoting cell proliferation and migration by targeting these lncRNAs or overexpressing the miRNAs.
One-sentence paraphrase of the abstract; not a substitute for reading it. No clinical advice. How this works
Abstract
Endometriosis has been increasingly associated with the aberrant regulation of non-coding RNAs (ncRNAs), particularly long non-coding RNAs (lncRNAs) and microRNAs (miRNAs). Despite the growing recognition of their biological significance, the precise molecular mechanisms and functional roles of lncRNAs LINC01140 and LINC01550 in the pathogenesis of endometriosis remain largely unexplored. In this study, we performed an integrative bioinformatics analysis utilizing the Gene Expression Omnibus dataset to systematically identify differentially expressed lncRNAs, miRNAs, and messenger RNAs (mRNAs), thereby constructing a comprehensive competing endogenous RNA (ceRNA) regulatory network. Primary endometrial stromal cells were meticulously isolated from ectopic and ovarian endometriotic lesions, and the RNA expression profiles were rigorously validated through RT-PCR. The subcellular localization of lncRNAs was precisely determined using fluorescence in situ hybridization, while the molecular interactions between lncRNAs and miRNAs were elucidated through dual-luciferase reporter assays. To delineate the functional impact, we conducted a series of assays including Western blot analysis to evaluate cellular proliferation, migration, and apoptotic processes. Our findings reveal that the LINC01140/miR-200c-3p and LINC01550/miR-363-3p regulatory networks are markedly upregulated in the cytoplasmic compartment of endometriotic cells, exerting pivotal roles in the progression of the disease. Importantly, the targeted silencing of lncRNAs or the overexpression of miR-363-3p/miR-200c-3p significantly attenuated cellular proliferation and migration, while concurrently inducing apoptosis. These results provide compelling evidence for the critical regulatory mechanisms orchestrated by lncRNAs in endometriosis, thereby establishing a robust theoretical framework for the development of innovative therapeutic interventions targeting ncRNA-mediated pathways.
My notes (saved in your browser only)
Condition tags
MeSH descriptors
Citation neighborhood
Papers in the corpus that this work cites (lower rings, blue) and that cite this one (upper rings, green). Dot size scales with the paper's in-corpus citation count — bigger dot = more influential within the endo/adeno field. Click a dot to open that paper. [ expand to 2 hops ] — adds papers reached through this work's immediate citers/citees. Heavier; up to 60 extra dots.
References (40)
- Challenges in endometriosis miRNA studies — From tissue heterogeneity to disease specific miRNAs via openalex
- Circ_0007331 knock‐down suppresses the progression of endometriosis via miR‐200c‐3p/HiF‐1α axis via openalex
- Disturbed progesterone signalling in an advanced preclinical model of endometriosis via openalex
- Effects of CDKN2B-AS1 on cellular proliferation, invasion and AKT3 expression are attenuated by miR-424-5p in a model of ovarian endometriosis via openalex
- Genetic or Enzymatic Disruption of Aromatase Inhibits the Growth of Ectopic Uterine Tissue via openalex
- Immunotherapy: A promising novel endometriosis therapy via openalex
- Impaired Localization of Claudin-11 in Endometriotic Epithelial Cells Compared to Endometrial Cells via openalex
- Integrated bioinformatic analysis of dysregulated microRNA-mRNA co-expression network in ovarian endometriosis via openalex
- LINC01018 and SMIM25 sponged miR-182-5p in endometriosis revealed by the ceRNA network construction via openalex
- LINC01116 promotes proliferation and migration of endometrial stromal cells by targeting FOXP1 via sponging miR‐9‐5p in endometriosis via openalex
- LINC01541 Functions as a ceRNA to Modulate the Wnt/β-Catenin Pathway by Decoying miR-506-5p in Endometriosis via openalex
- Local estrogen formation and its regulation in endometriosis via openalex
- Long noncoding RNA ADAMTS9-AS1 represses ferroptosis of endometrial stromal cells by regulating the miR-6516-5p/GPX4 axis in endometriosis via openalex
- Long noncoding RNAs in endometriosis: Biological functions, expressions, and mechanisms via openalex
- Nonsteroidal antiinflammatory drugs differentially suppress endometriosis in a murine model via openalex
- P450Arom induction in isolated control endometrial cells by peritoneal fluid from women with endometriosis via openalex
- Regulation of Inflammation Pathways and Inflammasome by Sex Steroid Hormones in Endometriosis via openalex
- Targeting delivery of mifepristone to endometrial dysfunctional macrophages for endometriosis therapy via openalex
- The expression of estrogen receptors as well as GREB1, c-MYC, and cyclin D1, estrogen-regulated genes implicated in proliferation, is increased in peritoneal endometriosis via openalex
- The landscape of non-coding RNAs in the immunopathogenesis of Endometriosis via openalex
- The Role of Long Non-Coding RNAs in Endometriosis via openalex
- W6804038101 via openalex
- W2525370412 via openalex
- W3106887675 via openalex
- W3129818825 via openalex
- W3162137154 via openalex
- W3187165599 via openalex
- W3195823357 via openalex
- W4221114134 via openalex
- W4296161377 via openalex
- W4306385621 via openalex
- W4308558977 via openalex
- W4362705041 via openalex
- W4376609273 via openalex
- W4387788571 via openalex
- W4393359065 via openalex
- W4400922274 via openalex
- W4402952231 via openalex
- W6664125244 via openalex
- W6753888907 via openalex
Source provenance
- europepmc
- last seen: 2026-06-19T06:14:56.452680+00:00
- openalex
- last seen: 2026-06-10T17:14:06.276822+00:00
- pubmed
- last seen: 2026-06-19T06:11:27.571367+00:00
License: CC0
· commercial use OK