Association of serum steroids with survival in metastatic hormone-sensitive prostate cancer.

IF 4.6 Endocrine-related cancer Pub Date : 2025-01-10 Print Date: 2025-02-01 DOI:10.1530/ERC-24-0140
Elahe A Mostaghel, Victoria Wang, Brett T Marck, Nima Sharifi, Alvin M Matsumoto, Christopher J Sweeney
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Abstract

The CHAARTED study showed that adding docetaxel (Doc) to androgen deprivation therapy (ADT) in men initiating treatment for metastatic hormone-sensitive prostate cancer (mHSPC) prolongs survival, particularly in high-volume disease. Androgens drive both mHSPC and metastatic castration-resistant prostate cancer (mCRPC). Lower nadir serum testosterone concentrations are associated with better outcomes in men treated with ADT for biochemical relapse, while higher androgens at mCRPC are associated with better prognosis and increased benefit from abiraterone. We evaluated the association of serum steroids at 24 weeks with overall survival (OS) and time to CRPC (TTCRPC) in 588 men with available samples from the CHAARTED study. Steroid concentrations were measured using mass spectrometry. The median testosterone concentration at 24 weeks was 8 ng/dL and did not differ in ADT alone vs ADT plus Doc arm. Achieving nadir testosterone below 20 ng/dL was not associated with OS or TTCRPC in either arm. In high-volume disease, Doc conferred an OS and TTCRPC benefit regardless of steroid concentrations. In low-volume disease, steroid concentrations in the lowest quartile at 24 weeks identified a subset of men with poor survival outcomes more like high-volume disease, and in whom Doc was also associated with improved OS and TTCRPC. The known OS benefit of Doc in high-volume mHSPC is not modified by serum steroid concentrations achieved on treatment. In low-volume disease, steroid concentrations in the lowest quartile may identify a poor prognosis subset in whom Doc also confers OS benefit.

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血清类固醇与对激素敏感的转移性前列腺癌患者生存期的关系。
CHAARTED 研究表明,在开始治疗转移性激素敏感性前列腺癌(mHSPC)的男性患者中,在雄激素剥夺疗法(ADT)的基础上添加多西他赛(Doc)可延长患者的生存期,尤其是在高发疾病中。雄激素对 mHSPC 和转移性阉割耐药前列腺癌(mCRPC)都有促进作用。在因生化复发而接受 ADT 治疗的男性中,较低的血清睾酮 (T) 浓度与较好的预后有关,而在 mCRPC 中,较高的雄激素与较好的预后和阿比特龙带来的更多益处有关。我们评估了 CHAARTED 研究中可获得样本的 588 名男性在 24 周时血清类固醇与总生存期 (OS) 和 CRPC (TTCRPC) 时间的关系。类固醇浓度采用质谱法进行测量。24周时的T浓度中位数为8 ng/dl,单用ADT与ADT加Doc治疗组之间没有差异。在两组中,达到低于20ng/dl的低水平T均与OS或TTCRPC无关。在高容量疾病中,无论类固醇浓度如何,Doc 都能带来 OS 和 TTCRPC 的益处。在低容量疾病中,第 24 周时类固醇浓度处于最低四分位数的男性子集的生存结果较差,更类似于高容量疾病,而 Doc 也与这些男性子集的 OS 和 TTCRPC 改善相关。在高容量 mHSPC 中,Doc 的已知 OS 益处不会因治疗时达到的血清类固醇浓度而改变。在低体积疾病中,类固醇浓度最低的四分位数可能会识别出预后较差的亚群,Doc 也能使这些亚群的 OS 受益。
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