What question did this study set out to answer?

The research aims to uncover the molecular mechanisms contributing to fibrosis in intrauterine adhesions (IUA).

April 13, 2026Open Access

Unraveling the fibrotic microenvironment in intrauterine adhesions through integrated metabolomics and proteomics

Key Points

The research aims to uncover the molecular mechanisms contributing to fibrosis in intrauterine adhesions (IUA).
Analyzed fibrotic tissues from 35 IUA patients and 20 normal controls.
Conducted metabolomic profiling using UPLC-MS.
Performed proteomic analysis with label-free quantitative mass spectrometry.
Identified differential metabolites and proteins through statistical analysis.
Explored pathway alterations using KEGG enrichment and integrated correlation analyses.
Identified 565 differential metabolites, primarily including lipids and organic acids.
Detected 2763 differential proteins with upregulation in focal adhesion pathways.
Notable correlations found between metabolites and fibrosis-related proteins.
Fumarate showed strong negative correlation with COL18A1 and positive correlation with E-cadherin.

Abstract

Intrauterine adhesions (IUA) result from endometrial basal layer injury, leading to fibrous tissue formation and impaired fertility. Current treatments fail to fully reverse the fibrotic microenvironment. This study aimed to elucidate molecular mechanisms underlying IUA-associated fibrosis through integrated metabolomics and proteomics. Fibrotic tissues from 35 moderate-to-severe IUA patients and normal endometrial samples from 20 controls were collected during hysteroscopy. Metabolomic profiling was performed using UPLC-MS, and proteomic analysis using label-free quantitative mass spectrometry. Differential metabolites (DEMs) and proteins (DEPs) were identified via OPLS-DA and statistical criteria (VIP > 1, P < 0.05 for DEMs; FDR-adjusted P < 0.05, FC ≥ 2 or ≤ 0.5 for DEPs). KEGG enrichment and integrated correlation analyses were conducted to explore pathway alterations and metabolite-protein interactions. A total of 565 DEMs were identified, primarily lipids, organic acids, and organooxygen compounds. KEGG enrichment revealed significant alterations in carbohydrate and amino acid metabolism pathways, with downregulation of TCA cycle intermediates and upregulation of glucose-6-phosphate, arginine, and methionine sulfoxide. Proteomics identified 2763 DEPs, with up-regulated proteins enriched in focal adhesion and ECM-receptor interaction pathways, and down-regulated proteins in DNA replication and complement cascades. Integrative analysis showed that carbohydrate and amino acid metabolism-related DEMs correlated negatively with fibrosis-related DEPs (e.g., collagens, TGF-β-related proteins), while focal adhesion-related DEPs correlated positively with fibrosis markers. Notably, fumarate showed strong negative correlations with COL18A1 (r=-0.71) and positive correlation with E-cadherin (r = 0.61). This multi-omics study reveals that metabolic reprogramming, particularly involving glycolysis and amino acid metabolism, is closely associated with activation of the integrin-focal adhesion signaling pathway in IUA fibrosis. These findings provide new insights into potential therapeutic targets for endometrial repair and fertility preservation.

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Unraveling the fibrotic microenvironment in intrauterine adhesions through integrated metabolomics and proteomics

Key Points

Abstract

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