Hematology Oncology Division, Department of Medicine, Beth Israel Deaconess Medical Center and Harvard Medical School, Boston, Massachusetts 02215, USA.
Endocr Relat Cancer. 2011 Aug 30;18(5):R175-82. doi: 10.1530/ERC-10-0339. Print 2011 Oct.
The majority of prostate cancers (PCa) express high levels of androgen receptor (AR) and are dependent for their growth on testosterone produced by the testes, which is reduced in the prostate to the higher affinity ligand 5α-dihydrotestosterone (DHT). PCa growth can be suppressed by androgen deprivation therapy, which involves removal of testicular androgens (surgical or medical castration) or treatment with an AR antagonist (or a combination of both), but patients invariably relapse with tumors that have been termed castration recurrent/resistant PCa (CRPC). Importantly, AR transcriptional activity becomes reactivated at this CRPC stage of the disease and remains essential for tumor growth. The objective of this review is to outline one clinically important mechanism contributing to this AR reactivation, which is increased intratumoral synthesis of testosterone and DHT from weak androgens produced by the adrenal glands and possibly de novo from cholesterol. Early studies showed that a substantial fraction of CRPC patients responded to adrenalectomy or medical suppression of adrenal androgen synthesis using agents such as ketoconazole (CYP17A1 inhibitor), and a recent phase III study of a more potent and selective CYP17A1 inhibitor (abiraterone) has demonstrated an improvement in survival. With the pending FDA approval of abiraterone for CRPC, defining the molecular mechanisms contributing to CYP17A1 inhibitor resistance/relapse and AR reactivation is now critical to build on these advances.
大多数前列腺癌 (PCa) 表达高水平的雄激素受体 (AR),并且依赖于睾丸产生的睾酮来生长,睾丸产生的睾酮在前列腺中被转化为亲和力更高的配体 5α-二氢睾酮 (DHT)。通过雄激素剥夺疗法可以抑制 PCa 的生长,该疗法包括去除睾丸雄激素(手术或药物去势)或用 AR 拮抗剂治疗(或两者结合),但患者总是会复发,形成被称为去势复发/耐药性 PCa (CRPC) 的肿瘤。重要的是,在疾病的 CRPC 阶段,AR 转录活性重新被激活,并且仍然是肿瘤生长所必需的。本综述的目的是概述导致这种 AR 重新激活的一个临床重要机制,即肿瘤内从肾上腺产生的弱雄激素和可能从头胆固醇中合成睾酮和 DHT 的增加。早期研究表明,相当一部分 CRPC 患者对肾上腺切除术或使用酮康唑(CYP17A1 抑制剂)等药物抑制肾上腺雄激素合成有反应,最近一项针对更有效和选择性 CYP17A1 抑制剂 (阿比特龙) 的 III 期研究表明,生存得到了改善。随着 abiraterone 即将获得 FDA 批准用于 CRPC,确定导致 CYP17A1 抑制剂耐药/复发和 AR 重新激活的分子机制对于利用这些进展至关重要。