What question did this study set out to answer?

This research aims to uncover the mechanism by which dihydroartemisinin influences ferroptosis and impacts steroid-induced osteonecrosis of the femoral head.

March 25, 2026Open Access

Computational and Experimental Biology Reveals Dihydroartemisinin’s Efficacy Against Steroid-Induced Osteonecrosis of the Femoral Head Adjusting Ferroptosis via CCL17-PRDX6

Key Points

This research aims to uncover the mechanism by which dihydroartemisinin influences ferroptosis and impacts steroid-induced osteonecrosis of the femoral head.
Utilized Mendelian randomization to analyze data from public databases.
Conducted animal experiments and transcriptomics sequencing to validate signaling pathways.
Employed computer-aided drug design to evaluate binding affinity of dihydroartemisinin to core targets.
Transcriptomics sequencing indicated dihydroartemisinin treats osteonecrosis by regulating ferroptosis.
Identified 564 ferroptosis-related targets and 1812 plasma proteins from the UK Biobank.
Found two quantitative trait loci causally linked to ferroptosis targets and 110 associated with plasma proteins.
Mediation analysis revealed 7 pathways, identifying 8 key targets, including CCL17 and PRDX6.

Abstract

Objective: According to existing research findings, dihydroartemisinin effectively regulates bone metabolism balance, while ferroptosis is closely related to the occurrence of steroid-induced osteonecrosis of the femoral head. As the exact biological mechanism among the three is still unclear, Mendelian randomization, computer-aided drug design, and transcriptomics sequencing were used to explore the specific mechanism of action. Methods: The study validated the specific signaling pathways through which dihydroartemisinin may treat steroid-induced osteonecrosis of the femoral head using animal experiments and transcriptomics sequencing. Data were obtained from public databases for Mendelian randomization analysis, and a two-sample Mendelian randomization was used to determine the intermediary role of core pathway-related targets. Computer-aided drug design was employed to assess the binding affinity between dihydroartemisinin and core targets. Results: Transcriptome sequencing determined that dihydroartemisinin may treat steroid-induced osteonecrosis of the femoral head by regulating ferroptosis. We obtained 564 ferroptosis-related targets that met the analysis criteria and 1812 plasma proteins from the UK Biobank, and analyzed finngenR11OSTEONDRUGS in the Finnish database as outcome. The results showed that there were two quantitative trait loci that had a causal relationship with ferroptosis targets. There were 110 protein quantitative trait loci causally associated with plasma proteins from the UK Biobank, and none of these loci had an inverse causal relationship with SONFH. Through mediation analysis, 7 mediating pathways were identified, yielding eight targets including ZP3, CCL17, APOE, C7ORF50, SPINK4, SPINK2, FTMT, and PRDX6. Computer-aided drug design revealed that CCL17 and PRDX6 exhibited the best docking effects. Conclusion: The study determined that CCL17 and PRDX6 have a significant causal relationship with SONFH. It also clarified the specific mechanism by which DHA may regulate ferroptosis to treat SONFH, which will provide a reference for the discussion of the prevention and treatment mechanisms of SONFH. Keywords: dihydroartemisinin, steroid-induced osteonecrosis of femoral head, ferroptosis, Mendelian randomization, computer-aided drug design

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Cite This Study

Li et al. (Sun,) studied this question.

synapsesocial.com/papers/69c37acab34aaaeb1a67c97e https://doi.org/https://doi.org/10.2147/dddt.s574294

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