手术或放疗治疗的临床局限性前列腺癌的辅助治疗。

Adjuvant therapy for clinical localized prostate cancer treated with surgery or irradiation.

作者信息

Schmidt J D, Gibbons R P, Murphy G P, Bartolucci A

机构信息

University of California San Diego School of Medicine, La Jolla, USA.

出版信息

Eur Urol. 1996;29(4):425-33. doi: 10.1159/000473791.

DOI:10.1159/000473791

PMID:8791049

Abstract

OBJECTIVE

Because of efficacy demonstrated with chemotherapy in patients with metastatic disease, the National Prostate Cancer Project in 1978 initiated two protocols evaluating adjuvant therapy following surgery (Protocol 900) and irradiation (Protocol 1000) for patients with localized disease at high risk for relapse.

METHODS

All patients underwent staging pelvic lymph node dissection. Following definitive treatment, patients were randomized to either cyclophosphamide 1 g/m2 intravenously every 3 weeks for 2 years, estramustine phosphate 600 mg/m2 orally daily for 2 years or to observation only. Accession closed in 1985 and included 184 patients in Protocol 900 (170 evaluable) and 253 in Protocol 1000 (233 evaluable).

RESULTS

Nodal involvement was identified in 198 patients (49% of total): 29% in Protocol 900 and 63% in protocol 1000. Median progression-free survival (PFS) and survival have been greater for patients in Protocol 900 regardless of adjuvant, reflecting their lower pathologic stage. Median PFS is significantly greater for patients in Protocol 1000 receiving estramustine (52.2 months) compared to cyclophosphamide (35.0 months). Median PFS for patients with nodal involvement in Protocol 1000 receiving estramustine is increased (43.5 months) compared to no treatment (21.5 months). Patients with limited nodal involvement in Protocol 1000 have a longer median PFS (45.6 months) compared to patients with extensive disease (23.6 months). But in the latter group patients receiving estramustine experienced a significantly longer median PFS (43.5 months) compared to cyclophosphamide (29.1 months) or no adjuvant (13.5 months). Increased PFS with estramustine adjuvant was also noted in stage C patients (only Protocol 900) and in those with high-grade (grade 3) tumors (both protocols).

CONCLUSIONS

With now over 10 years mean follow-up for this series of patients, we conclude that adjuvant estramustine is beneficial for prostate cancer patients receiving definitive irradiation. This benefit is particularly noted in those patients with extensive nodal involvement (N+, D-1).

摘要

目的

鉴于化疗对转移性疾病患者已显示出疗效，1978年国家前列腺癌项目启动了两项方案，评估对复发风险高的局限性疾病患者术后（方案900）和放疗后（方案1000）的辅助治疗。

方法

所有患者均接受盆腔淋巴结清扫分期。在确定性治疗后，患者被随机分为三组，分别是每3周静脉注射环磷酰胺1 g/m²，共2年；口服磷酸雌莫司汀600 mg/m²，每日一次，共2年；或仅进行观察。入组于1985年结束，方案900纳入184例患者（170例可评估），方案1000纳入253例患者（233例可评估）。

结果

198例患者（占总数的49%）发现有淋巴结受累：方案900中为29%，方案1000中为63%。无论是否接受辅助治疗，方案900中的患者无进展生存期（PFS）和总生存期的中位数均更长，这反映了他们较低的病理分期。方案1000中接受磷酸雌莫司汀治疗的患者的中位PFS（52.2个月）显著长于接受环磷酰胺治疗的患者（35.0个月）。方案1000中接受磷酸雌莫司汀治疗的有淋巴结受累患者的中位PFS（43.5个月）相较于未治疗患者（21.5个月）有所增加。方案1000中淋巴结受累局限的患者的中位PFS（45.6个月）长于广泛受累患者（23.6个月）。但在后一组中，接受磷酸雌莫司汀治疗的患者的中位PFS（43.5个月）显著长于接受环磷酰胺治疗的患者（29.1个月）或未接受辅助治疗的患者（13.5个月）。在C期患者（仅方案900）和高级别（3级）肿瘤患者（两个方案）中也观察到磷酸雌莫司汀辅助治疗使PFS增加。