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Epigenetic alterations of AKT1 orchestrate a metabolic reprogramming in advanced lipedema: translational insights from an integrated multi-omics study
Resource type
Authors/contributors
- Santella, Biagio (Author)
- Salvati, Annamaria (Author)
- Papp, Alexander (Author)
- D'Ursi, Annamaria (Author)
- Memoli, Domenico (Author)
- Mingo, Monica (Author)
- Pulai, Christoph (Author)
- Marino, Carmen (Author)
- Rastrelli, Luca (Author)
- D'Elia, Maria (Author)
- Nassa, Giovanni (Author)
- Schiavo, Luigi (Author)
Title
Epigenetic alterations of AKT1 orchestrate a metabolic reprogramming in advanced lipedema: translational insights from an integrated multi-omics study
Abstract
BACKGROUND: lipedema is a chronic, progressive adipose disorder predominantly affecting women, characterized by painful, symmetrical subcutaneous fat accumulation, and typically resistant to lifestyle interventions. The pathophysiology of advanced-stage lipedema remains poorly defined, and no validated biomarkers or targeted therapies are currently available.
METHODS: in this observational study, we applied a comprehensive multi-omics approach to dissect the molecular and metabolic alterations underlying late-stage lipedema.
RESULTS: Genome-wide DNA methylation profiling identified over 5,000 differentially methylated CpG sites affecting genes involved in receptor tyrosine kinase signaling, phospho-metabolism, and immune pathways. Transcriptomic analysis revealed profound downregulation of mitochondrial functions, including oxidative phosphorylation, the TCA cycle, and fatty acid β-oxidation, alongside disruption of the sirtuin pathway and extracellular matrix remodeling. Integrative analysis pinpointed AKT1 as a central regulatory node: its promoter region was hypomethylated, correlating with increased gene expression and protein phosphorylation. Metabolomic profiling confirmed AKT1-linked metabolic dysregulation, including altered levels of L-arginine, NADP+, ATP, guanosine, glycerol, and glutamate, indicating impaired redox balance and energy metabolism. Trans-omic network analysis positioned AKT1 at the intersection of multiple dysregulated pathways, suggesting its key role in advanced-stage lipedema.
CONCLUSIONS: the consistent enhancing of AKT pathway signaling across omic layers highlights its potential not only as a biomarker for disease stratification but also as a putative druggable target for therapeutic intervention. These findings offer new mechanistic insights into lipedema pathophysiology and provide a rationale for future personalized treatment strategies guided by AKT1-centric molecular profiling.
Publication
Journal of Translational Medicine
Date
2026-01-24
Journal Abbr
J Transl Med
PMID
41580786
ISSN
1479-5876
Short Title
Epigenetic alterations of AKT1 orchestrate a metabolic reprogramming in advanced lipedema
Language
eng
Library Catalog
PubMed
Citation
Santella, B., Salvati, A., Papp, A., D’Ursi, A., Memoli, D., Mingo, M., Pulai, C., Marino, C., Rastrelli, L., D’Elia, M., Nassa, G., & Schiavo, L. (2026). Epigenetic alterations of AKT1 orchestrate a metabolic reprogramming in advanced lipedema: translational insights from an integrated multi-omics study. Journal of Translational Medicine. https://doi.org/10.1186/s12967-026-07726-w
Topic
Publication
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