Identify the therapeutic role and potential mechanism of α-cyperone in diminished ovarian reserve based on network pharmacology, molecular docking, Lip-MS and experimental validation
Jingwen Guo, Xitang Yang, Xue Chen, Rong Hu, Hua Guo

TL;DR
This study explores how α-cyperone may help treat diminished ovarian reserve by targeting key proteins and reversing gene expression changes.
Contribution
This is the first study to investigate the therapeutic potential and mechanism of α-cyperone in treating diminished ovarian reserve using network pharmacology and experimental validation.
Findings
α-cyperone binds strongly to 22 key proteins linked to DOR and improves granule cell function.
Lip-MS confirmed α-cyperone's binding to MAP2K1, GSK3B, and MAPK14, reversing gene expression patterns.
The compound enhances cell viability and reduces oxidative stress in a DOR cell model.
Abstract
The presence of diminished ovarian reserve (DOR) poses a significant threat to female fertility, with no current effective treatment available. Inflammation plays pivotal roles in the pathogenesis of DOR. α-Cyperone (AC) exhibits notable anti-inflammatory and anti-oxidative properties; however, its potential for improving DOR remains unexplored. The PubChem, PharmMapper, and SwissTargetForecast databases were queried to retrieve biochemical information and drug targets for AC. The identification of disease targets for DOR involved referring to the OMIM and Genecards databases. AC’s therapeutic targets against DOR were determined by examining the overlap between drug targets and disease targets. To analyze GO function enrichment, KEGG pathway, and disease association, the Metascape database was utilized. The results were then visualized using Cytoscape software. Receptor-ligand…
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Taxonomy
TopicsReproductive Biology and Fertility · Ovarian function and disorders · Ovarian cancer diagnosis and treatment
