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Obacunone 通过抑制雄激素受体二聚化改善二氢睾酮诱导的雄激素性脱发。

Obacunone improves dihydrotestosterone-induced androgen alopecia by inhibiting androgen receptor dimerization.

机构信息

China Pharmaceutical University, PR China.

China Pharmaceutical University, PR China.

出版信息

Phytomedicine. 2024 Dec;135:156042. doi: 10.1016/j.phymed.2024.156042. Epub 2024 Sep 14.

DOI:10.1016/j.phymed.2024.156042
PMID:39306884
Abstract

BACKGROUND

Dihydrotestosterone-induced androgen receptor activation and nuclear translocation was identified as the key event in androgen alopecia, which led to dermal papilla cell damage and hair growth cycle arrest. Inhibiting androgen receptor activation or nuclear translocation thus represents a potential therapeutic strategy for reducing dermal papilla cell damage and treating androgen alopecia.

PURPOSE

To evaluate the effects of obacunone androgen alopecia and explore the potential underlying mechanisms.

METHODS

The effects of obacunone on androgen receptor activation and changes in the properties of dermal papilla cells were investigated. Meanwhile, the effects of obacunone on transforming growth factor-β-induced hair follicle stem cell damage and on androgen alopecia mice induced by dihydrotestosterone were evaluated.

RESULTS

Obacunone can competitively bind to androgen receptors with dihydrotestosterone, thereby alleviating the androgen receptor dimerization and nuclear translocation. The negative effects of dihydrotestosterone on dermal papilla cell apoptosis, senescence, and cycle arrest were alleviated by obacunone. Obacunone also counteracted the proliferation and apoptosis of transforming growth factor-β-mediated hair follicle stem cells. In mice with androgen alopecia, treatment with obacunone promoted mice hair growth and inhibited TGF-β/smad signaling.

CONCLUSION

Thus, inhibiting androgen receptor dimerization was found to be an effective strategy for alleviating androgen alopecia. Obacunone follows a novel mechanism and holds potential as a drug candidate for androgen alopecia through inhibition of the dimerization of the androgen receptor. This targeting strategy may provide a new avenue for the development of new drugs different from the existing therapeutic approaches.

摘要

背景

双氢睾酮诱导的雄激素受体激活和核转位被认为是雄激素性脱发的关键事件,导致真皮乳头细胞损伤和毛发生长周期停滞。因此,抑制雄激素受体激活或核转位代表了减少真皮乳头细胞损伤和治疗雄激素性脱发的一种潜在治疗策略。

目的

评估obacunone 对雄激素性脱发的影响,并探讨其潜在的作用机制。

方法

研究了obacunone 对雄激素受体激活和真皮乳头细胞特性变化的影响。同时,评估了 obacunone 对转化生长因子-β诱导的毛囊干细胞损伤和双氢睾酮诱导的雄激素性脱发小鼠的作用。

结果

obacunone 可以与双氢睾酮竞争结合雄激素受体,从而减轻雄激素受体二聚化和核转位。obacunone 减轻了双氢睾酮对真皮乳头细胞凋亡、衰老和周期阻滞的负面影响。obacunone 还拮抗了转化生长因子-β介导的毛囊干细胞增殖和凋亡。在雄激素性脱发小鼠中,obacunone 治疗促进了小鼠毛发的生长,并抑制了 TGF-β/smad 信号通路。

结论

因此,抑制雄激素受体二聚化被发现是缓解雄激素性脱发的有效策略。obacunone 通过抑制雄激素受体二聚化,遵循一种新的机制,有望成为一种治疗雄激素性脱发的药物候选物。这种靶向策略可能为开发与现有治疗方法不同的新药提供新途径。

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