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甾体激素的双重功能:在前列腺癌治疗中的意义。

The bifunctional role of steroid hormones: implications for therapy in prostate cancer.

出版信息

Oncology (Williston Park). 2014 May;28(5):397-404.

Abstract

Ablation of the androgen-signaling axis is currently a dominant theme in developmental therapeutics in prostate cancer. Highly potent inhibitors of androgen biosynthesis and androgen receptor (AR) function have formally improved survival in castration-resistant metastatic disease. Resistance to androgen-ablative strategies arises through diverse mechanisms. Strategies to preserve and extend the success of hormonal therapy while mitigating the emergence of resistance have long been of interest. In preclinical models, intermittent hormonal ablative strategies delay the emergence of resistant stem-cell-driven phenotypes, but clinical studies in hormone-naive disease have not observed more than noninferiority over continual androgen ablation. In castration-resistant disease, response and improvement in subjective quality of life with therapeutic testosterone has been observed, but so too has symptomatic and life-threatening disease acceleration. The multifunctional and paradoxical role of steroid hormones in regulating proliferation and differentiation, as well as cell death, requires deeper understanding. The lack of molecular biomarkers that predict the outcome of hormone supplementation in a particular clinical context remains an obstacle to individualized therapy. Biphasic patterns of response to hormones are identifiable in vitro, and endocrine-regulated neoplasms that proliferate after prolonged periods of hormone deprivation appear preferentially sex steroid-suppressible. This review examines the relevance of a translational framework for studying therapeutic androgens in prostate cancer.

摘要

雄激素信号轴的消融目前是前列腺癌发展治疗学中的一个主要主题。雄激素生物合成和雄激素受体 (AR) 功能的高效抑制剂已正式改善了去势抵抗转移性疾病的生存率。通过多种机制产生了对雄激素消融策略的抵抗。长期以来,人们一直关注保留和延长激素治疗成功的同时减轻耐药性出现的策略。在临床前模型中,间歇性激素消融策略延迟了耐药性干细胞驱动表型的出现,但在激素初治疾病的临床研究中,与持续雄激素消融相比,并未观察到非劣效性。在去势抵抗疾病中,治疗性睾丸激素治疗可观察到应答和主观生活质量的改善,但也观察到症状性和危及生命的疾病加速。甾体激素在调节增殖和分化以及细胞死亡方面的多功能和矛盾作用需要更深入的了解。缺乏预测特定临床环境下激素补充治疗结果的分子生物标志物仍然是个体化治疗的障碍。体外可识别激素的双相反应模式,并且在长时间激素剥夺后增殖的内分泌调节肿瘤似乎更能抑制性激素。这篇综述探讨了在前列腺癌中研究治疗性雄激素的转化框架的相关性。

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