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多西他赛、雌莫司汀以及对前列腺癌进行确定性局部治疗后前列腺特异性抗原进展的男性患者进行15个月雄激素剥夺治疗。

Docetaxel, estramustine, and 15-month androgen deprivation for men with prostate-specific antigen progression after definitive local therapy for prostate cancer.

作者信息

Taplin Mary-Ellen, Xie Wanling, Bubley Glenn J, Ernstoff Marc S, Walsh William, Morganstern Daniel E, Regan Meredith M

机构信息

Dana-Farber Cancer Institute, Boston, MA 02115, USA.

出版信息

J Clin Oncol. 2006 Dec 1;24(34):5408-13. doi: 10.1200/JCO.2006.06.6589.

DOI:10.1200/JCO.2006.06.6589
PMID:17135641
Abstract

PURPOSE

Androgen-deprivation therapy (ADT) is effective for relapsed prostate cancer, but is rarely curative. The purpose of this trial was to determine the feasibility, toxicity, and prostate-specific antigen (PSA) response of chemotherapy and limited ADT for men with PSA relapse.

PATIENTS AND METHODS

Eligible men had an increasing PSA and no metastases after prostatectomy and/or radiation for localized disease. Treatment consisted of four cycles of docetaxel (70 mg/m2) every 21 days and estramustine 280 mg tid on days 1 through 5. After chemotherapy, goserelin acetate and bicalutamide were prescribed for 15 months.

RESULTS

Sixty-two patients were enrolled. A complete PSA response (CR) was defined as PSA at or below the assay-specific lower limit. The proportion of patients with CR after chemotherapy, after ADT, and at 1 year after completion of ADT was 53%, 63%, and 36%, respectively. Testosterone was more than 100 ng/dL (median, 250 ng/dL) 1 year after completion of ADT in 97% of patients. Patients with a PSA less than 3.0 ng/mL at enrollment had a significantly longer time to progression (TTP; P = .0004). Of 56 patients who were observed at least 1 year after completion of ADT, 23 (41%) have not experienced progression as of their last follow-up. The median TTP is 34 months from treatment initiation (maximum, 74 months free from progression).

CONCLUSION

Chemotherapy plus ADT was feasible for early prostate cancer relapse. Forty-one percent of men who are at least 1 year after completion of ADT with recovered testosterone have not experienced progression. This approach is being tested in a randomized trial with investigation of predictors of response.

摘要

目的

雄激素剥夺疗法(ADT)对复发性前列腺癌有效,但很少能治愈。本试验的目的是确定化疗联合有限疗程ADT用于前列腺特异性抗原(PSA)复发男性患者的可行性、毒性及PSA反应。

患者与方法

符合条件的男性患者在前列腺切除术后和/或针对局限性疾病进行放疗后PSA升高且无转移。治疗方案为每21天进行4个周期的多西他赛(70mg/m²)治疗,并在第1至5天每日3次给予雌莫司汀280mg。化疗后,给予醋酸戈舍瑞林和比卡鲁胺治疗15个月。

结果

共纳入62例患者。完全PSA缓解(CR)定义为PSA处于或低于检测方法特异性下限。化疗后、ADT后以及ADT完成后1年时CR患者的比例分别为53%、63%和36%。97%的患者在ADT完成后1年时睾酮水平高于100ng/dL(中位数为250ng/dL)。入组时PSA低于3.0ng/mL的患者进展时间(TTP)显著更长(P = 0.0004)。在ADT完成后至少观察1年的56例患者中,截至最后一次随访,有23例(41%)未出现疾病进展。从治疗开始计算的中位TTP为34个月(最长无进展生存期为74个月)。

结论

化疗联合ADT用于早期前列腺癌复发是可行的。在ADT完成后睾酮恢复且至少随访1年的男性患者中,41%未出现疾病进展。目前正在一项随机试验中对该方法进行测试,并研究反应预测因素。

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