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多西他赛或米托蒽醌治疗激素难治性前列腺癌:TAX-327研究中前列腺特异性抗原、疼痛、生活质量反应与生存之间的关系

Treatment of hormone-refractory prostate cancer with docetaxel or mitoxantrone: relationships between prostate-specific antigen, pain, and quality of life response and survival in the TAX-327 study.

作者信息

Berthold Dominik R, Pond Gregory R, Roessner Martin, de Wit Ronald, Eisenberger Mario, Tannock And Ian F

机构信息

Princess Margaret Hospital and University of Toronto, Toronto, Ontario, Canada.

出版信息

Clin Cancer Res. 2008 May 1;14(9):2763-7. doi: 10.1158/1078-0432.CCR-07-0944.

DOI:10.1158/1078-0432.CCR-07-0944
PMID:18451243
Abstract

PURPOSE

The TAX-327 study randomized 1,006 men with metastatic hormone-refractory prostate cancer to receive 3-weekly docetaxel, weekly docetaxel, or mitoxantrone, each with prednisone.

EXPERIMENTAL DESIGN

We used the TAX-327 database to address (a) the relationship between quality of life (QoL) and pain; (b) whether minimally symptomatic patients benefit from treatment or have treatment-related decline in QoL; (c) the relationships between prostate-specific antigen (PSA) response, pain response, and QoL response; (d) the times at which these responses are first observed; and (e) whether PSA, pain, and/or QoL response predict for overall survival.

RESULTS

At baseline, 374 of 815 men assessed for QoL had major pain; of these, 92% had substantial impairment of QoL compared with 75% without major pain (P < 0.001). Men with minimal symptoms had prolonged survival (median, 25.6 months) compared with symptomatic patients (median, 17.1 months; P = 0.009); they were more likely to have initial deterioration of QoL if treated with weekly docetaxel. PSA response and pain response, but not QoL response, were independently associated with survival in landmark analysis. Median times to PSA and pain response were 44 and 27 days, respectively; some men had initial increase in serum PSA before subsequent decline.

CONCLUSIONS

Symptoms other than pain contribute to impaired QoL in men with hormone-refractory prostate cancer. Those with minimal symptoms have prolonged survival. Both pain and PSA response are associated with survival but are not adequate to use as surrogate end points in phase 3 studies. Early increases in serum PSA (up to 12 weeks) should be ignored when determining response or progression.

摘要

目的

TAX - 327研究将1006例转移性激素难治性前列腺癌患者随机分为三组,分别接受每3周一次的多西他赛、每周一次的多西他赛或米托蒽醌治疗,每组均联合泼尼松。

实验设计

我们利用TAX - 327数据库来探讨以下问题:(a)生活质量(QoL)与疼痛之间的关系;(b)症状轻微的患者是否从治疗中获益或出现与治疗相关的生活质量下降;(c)前列腺特异性抗原(PSA)反应、疼痛反应和生活质量反应之间的关系;(d)首次观察到这些反应的时间;(e) PSA、疼痛和/或生活质量反应是否可预测总生存期。

结果

基线时,在815例接受生活质量评估的男性中,374例有重度疼痛;其中,与无重度疼痛者相比,92%的患者生活质量有严重受损,而无重度疼痛者这一比例为75%(P < 0.001)。与有症状的患者(中位生存期17.1个月;P = 0.009)相比,症状轻微的患者生存期延长(中位生存期25.6个月);若接受每周一次的多西他赛治疗,他们更有可能出现生活质量的初始恶化。在标志性分析中,PSA反应和疼痛反应与生存期独立相关,但生活质量反应与生存期无关。PSA反应和疼痛反应的中位时间分别为44天和27天;一些男性在血清PSA随后下降之前有初始升高。

结论

除疼痛外的其他症状也会导致激素难治性前列腺癌男性患者的生活质量受损。症状轻微的患者生存期延长。疼痛和PSA反应均与生存期相关,但不足以作为3期研究的替代终点。在确定反应或进展时,应忽略血清PSA在早期(长达12周)的升高。

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