Friend or foe? Deciphering androgen receptor action to improve bipolar androgen therapy for prostate cancer.

Endocrine-related cancer Pub Date : 2024-12-18 Print Date: 2025-01-01 DOI:10.1530/ERC-24-0208
Samuel P G Rollin, Mitchell G Lawrence, Anthony M Joshua, Luke A Selth
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Abstract

Inhibiting the activity of the androgen receptor (AR) is the cornerstone treatment for advanced prostate cancer. AR-targeted therapies are highly effective in slowing disease progression but are not curative. Failure of these therapies results in a disease state termed castration-resistant prostate cancer, which is associated with significant patient morbidity and mortality. In most cases, resistance to AR-targeted therapies arises due to alterations that reactivate the AR signalling axis. Interestingly, it has long been recognised that potent activation of AR with supraphysiological levels of androgens can suppress prostate cancer growth in both preclinical models and patients. This intriguing paradox, where both inhibition and activation of AR have anti-cancer effects, is now being harnessed clinically in the form of bipolar androgen therapy (BAT). This review describes mechanisms underlying the tumour-suppressive functions of AR in the context of potent androgenic stimulation and discusses how our maturing understanding of these processes is influencing the clinical deployment of BAT.

朋友还是敌人?解密雄激素受体作用,改进前列腺癌的双极雄激素疗法。
抑制雄激素受体(AR)的活性是治疗晚期前列腺癌的基础。AR靶向疗法在延缓疾病进展方面非常有效,但并不能治愈疾病,由此产生的疾病状态被称为阉割耐药前列腺癌,与患者的发病率和死亡率密切相关。在大多数情况下,对这些疗法的耐药性是由于重新激活 AR 信号轴的改变造成的。有趣的是,人们早已认识到,用超生理水平的雄激素强效激活 AR 可以抑制临床前模型和患者的前列腺癌生长。这种有趣的悖论--抑制和激活 AR 都具有抗癌作用--目前正以双极雄激素疗法 (BAT) 的形式在临床上得到利用。这篇综述描述了在强效雄激素刺激下AR抑制肿瘤功能的机制,并讨论了我们对这些机制日益成熟的理解如何影响BAT的临床应用。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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