Testosterone nadir and clinical outcomes in patients with advanced prostate cancer: Post hoc analysis of triptorelin pamoate Phase III studies

IF 1.6 Q3 UROLOGY & NEPHROLOGY BJUI compass Pub Date : 2024-01-10 DOI:10.1002/bco2.318

Laurence Klotz, Tri Tat

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Abstract

Objective

The objective of the study is to evaluate whether low nadir testosterone during treatment with triptorelin pamoate, a luteinising hormone-releasing hormone (LHRH) agonist, is associated with improved clinical outcomes in patients with advanced prostate cancer using a retrospective analysis of clinical trial data.

Patients and methods

Data were pooled from three prospective, 9–12-month Phase III studies of triptorelin monotherapy in patients with advanced prostate cancer (including NCT00751790). The serum testosterone concentration suppression targets evaluated were <0.35 nmol/L (<10 ng/dl), <0.7 nmol/L (<20 ng/dl), <1.7 nmol/L (<50 ng/dl) and ≥1.7 nmol/L. Overall survival (OS) and disease-specific survival (DSS) by testosterone suppression group were assessed by Kaplan–Meier analysis, with log-rank test. The time frame for the primary analysis was Days 1–518 (median OS follow-up 254 days [range, 29–518 days]) and for the sensitivity analyses was Days 1–262. Supplementary analyses combined the ≥0.7- to <1.7-nmol/L and ≥1.7-nmol/L groups.

Results

The sample size comprised 592 patients (most received triptorelin monotherapy; four reported concomitant androgen receptor-axis–targeted therapy). Nadir testosterones of <0.35, ≥0.35 to <0.7, ≥0.7 to <1.7 and ≥1.7 nmol/L were achieved by 96%, 3.2%, 0.34% and 0.17% of patients, respectively. Better OS with decreasing level of nadir testosterone was observed (p < 0.001) and this persisted after sensitivity/supplemental analyses (all p < 0.001). Differences in DSS with decreasing levels of nadir testosterone were not statistically significant in the primary analysis. Sensitivity/supplemental analysis showed better DSS with decreasing level of nadir testosterone (Days 1–262, p = 0.01; combined groups Days 1–518, p = 0.03; combined groups Days 1–262, p = 0.005).

Conclusion

Low nadir testosterone achieved during treatment with the LHRH agonist triptorelin was associated with improved OS and DSS in patients with advanced prostate cancer.

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晚期前列腺癌患者的睾酮最低值与临床疗效：帕莫酸曲普瑞林III期研究的事后分析

该研究的目的是通过对临床试验数据的回顾性分析，评估黄体生成素释放激素（LHRH）激动剂帕莫酸曲普瑞林治疗期间的低睾酮是否与晚期前列腺癌患者临床预后的改善有关。数据来自三项针对晚期前列腺癌患者的曲普瑞林单药治疗的前瞻性、为期9-12个月的III期研究（包括NCT00751790）。评估的血清睾酮浓度抑制目标为<0.35 nmol/L（<10 ng/dl）、<0.7 nmol/L（<20 ng/dl）、<1.7 nmol/L（<50 ng/dl）和≥1.7 nmol/L。睾酮抑制组的总生存期（OS）和疾病特异性生存期（DSS）通过卡普兰-梅耶分析和对数秩检验进行评估。主要分析的时间范围为第1-518天（中位OS随访254天[范围为29-518天]），敏感性分析的时间范围为第1-262天。补充分析合并了≥0.7-<1.7-nmol/L组和≥1.7-nmol/L组。样本量包括592例患者（大多数接受曲普瑞林单药治疗；4例报告同时接受雄激素受体轴靶向治疗）。96%、3.2%、0.34%和0.17%的患者体内睾酮含量分别为＜0.35、≥0.35至＜0.7、≥0.7至＜1.7和≥1.7 nmol/L。随着睾酮最低水平的降低，观察到更好的OS（p < 0.001），在进行敏感性/补充性分析后，这种情况依然存在（所有p < 0.001）。在主要分析中，随着最低睾酮水平的降低，DSS的差异无统计学意义。LHRH激动剂曲普瑞林治疗期间达到的低睾酮水平与晚期前列腺癌患者OS和DSS的改善有关。

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