连续与间歇性雄激素剥夺疗法治疗转移性前列腺癌。
Continuous vs. intermittent androgen deprivation therapy for metastatic prostate cancer.
机构信息
Department of Urology, Radboud University Nijmegen Medical Center, Nijmegen, the Netherlands.
出版信息
Urol Oncol. 2013 Jul;31(5):549-56. doi: 10.1016/j.urolonc.2011.03.008. Epub 2011 May 10.
OBJECTIVES
To analyze the predictive value of PSA for progression and the role of testosterone for quality of life (QOL) in patients with androgen deprivation therapy (ADT) for metastatic prostate cancer.
MATERIALS AND METHODS
PSA and testosterone data were used from a phase III trial randomizing patients without progression and PSA < 4 ng/ml (n = 193), after 6 months induction course, between continuous (CAD) (n = 96) and intermittent (IAD) (n = 97) ADT. The 2-year risk of progression was calculated for baseline PSA, 'fast' and 'slow' PSA decline to < 4 ng/ml (60 days cut-off), PSA nadir, performance status and pain. Testosterone kinetics and QOL were also evaluated. Univariate Kaplan Meier survival analysis and log rank tests were used to compare the risk of progression.
RESULTS
For progression analysis, 173 patients' data were available. The 2-year risk of progression for baseline PSA < 50 ng/ml, 50 to <500 ng/ml, and ≥ 500 ng/ml was 25%, 55%, and 76% (P = 0.03) in CAD, and 38%, 64%, and 85% (P = 0.006) in IAD, respectively. The 2-year risk of progression for PSA nadir ≤ 0.2 ng/ml, and > 0.2 to 4 ng/ml in CAD was 31% and 70% (P < 0.001), respectively. In the IAD group, a similar trend was seen. Patients with PSA nadir ≤ 0.2 ng/ml, though had significantly higher 2-year risk of progression compared to CAD (53% vs. 31% (P = 0.03), respectively. PSA decline showed no predictive value. Patients without pain had a significantly lower 2-year risk of progression in both groups. Without ADT testosterone remained at castrate level for 4 months. After the first and second IAD cycle 92% and 46%, respectively, had a normalized testosterone. No QOL difference was found, although more side effects occurred in CAD.
CONCLUSIONS
Metastatic prostate cancer patients with high baseline PSA, pain, and high PSA nadir have a poor prognosis with ADT. Patients with low PSA nadir do significantly worse with IAD compared with CAD. Low testosterone after ADT and incomplete testosterone recovery may explain similar QOL. Therefore, IAD is not a good treatment option for many metastatic prostate cancer patients.
目的
分析前列腺特异性抗原(PSA)对进展的预测价值,以及睾酮在接受去势治疗(ADT)的转移性前列腺癌患者中的生活质量(QOL)中的作用。
材料与方法
使用一项 III 期试验的数据,该试验将无进展且 PSA<4ng/ml(n=193)的患者随机分为连续(CAD)(n=96)和间歇性(IAD)(n=97)ADT 组,在 6 个月诱导期后进行分析。根据基线 PSA、PSA 快速和缓慢下降至<4ng/ml(60 天截止)、PSA 最低点、表现状态和疼痛,计算 2 年进展风险。还评估了睾酮动力学和 QOL。使用单变量 Kaplan-Meier 生存分析和对数秩检验比较进展风险。
结果
对于进展分析,173 名患者的数据可用。CAD 组中,基线 PSA<50ng/ml、50-<500ng/ml 和≥500ng/ml 的 2 年进展风险分别为 25%、55%和 76%(P=0.03),IAD 组中分别为 38%、64%和 85%(P=0.006)。CAD 组中,PSA 最低点≤0.2ng/ml 和>0.2-4ng/ml 的 2 年进展风险分别为 31%和 70%(P<0.001)。在 IAD 组中也观察到类似的趋势。PSA 最低点≤0.2ng/ml 的患者与 CAD 组相比,2 年进展风险显著更高(53%比 31%(P=0.03))。PSA 下降无预测价值。两组中无疼痛的患者 2 年进展风险显著降低。ADT 后,无睾酮仍保持在去势水平 4 个月。第一次和第二次 IAD 周期后,分别有 92%和 46%的患者睾酮正常。虽然 CAD 中发生更多副作用,但未发现 QOL 差异。
结论
基线 PSA、疼痛和 PSA 最低点高的转移性前列腺癌患者 ADT 预后较差。PSA 最低点低的患者接受 IAD 治疗时的预后明显比 CAD 更差。ADT 后低睾酮和不完全的睾酮恢复可能解释了相似的 QOL。因此,IAD 不是许多转移性前列腺癌患者的好治疗选择。
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