Dusenbery Kathryn E, Bellairs Ellen E, Potish Roger A, Twiggs Leo B, Boente Matthew P
Department of Therapeutic Radiology-Radiation Oncology, University of Minnesota Medical School, Minneapolis, MN 55455, USA.
Gynecol Oncol. 2005 Feb;96(2):307-13. doi: 10.1016/j.ygyno.2004.08.040.
The purpose of the present study is evaluation of the long-term efficacy of sequential abdominopelvic radiotherapy and melphalan in the management of ovarian carcinoma.
From 1970 to 1976, 94 women with stages I-III epithelial ovarian carcinoma enrolled in a prospective nonrandomized clinical trial were prescribed 20 Gy to the upper abdomen and 50 Gy to the pelvis followed by courses of melphalan (1 mg/kg/course). Primary endpoints were survival, recurrence, and toxicity.
There were 19 stage I, 25 stage II, and 50 stage III patients. For all stages, overall survival was 42% at 5 years, 30% at 10 years, and 17% at 25 years. Median follow-up of the survivors was 24 years. Disease-free survival was 48% at 5 years and remained at 45% from 10 to 25 years. All but two recurrences occurred within the first 27 months. No recurrence or treatment-related death occurred after 8 years. No recurrence was salvaged. All but one initial recurrence was within the peritoneal cavity. Of the 31 patients undergoing a second-look surgical procedure, 84% were free of tumor. Only 8% of patients recurred after a negative second look. Stage and the presence of palpable postoperative disease were significant prognostic factors. Disease-free survivals were 95% from 5 to 25 years for stage I, 70% at 5 years and 60% at 25 years for stage II, and 20% from 5 to 25 years for stage III (P < 0.0001). Although no patient with postoperative palpable tumor was cured, 25% lived beyond 2 years. Stage III patients without postoperative palpable tumor achieved a 47% 25-year disease-free survival. Acute toxicity was acceptable, and 98% of patients completed radiation therapy. Chronic toxicity included a 12% small bowel obstruction rate and a 3% fatal second malignancy/hematological toxicity rate (two cases of acute myelocytic leukemia, one case of thrombocytopenia).
The long-term disease-free survival obtained with abdominopelvic radiotherapy followed by single alkylating agent chemotherapy has not been exceeded by three subsequent decades of multiagent chemotherapy trials. Abdominal radiotherapy may be useful to consolidate complete responses following therapy multiagent chemotherapy, particularly with the upper abdominal dose escalation provided by intensity modulated radiation therapy and possibly in conjunction with chemotherapy.
本研究旨在评估序贯腹盆腔放疗与美法仑治疗卵巢癌的长期疗效。
1970年至1976年,94例I - III期上皮性卵巢癌患者参加了一项前瞻性非随机临床试验,接受上腹部20 Gy和盆腔50 Gy的放疗,随后进行美法仑疗程(1 mg/kg/疗程)。主要终点为生存率、复发率和毒性。
有19例I期、25例II期和50例III期患者。所有分期患者的5年总生存率为42%,10年为30%,25年为17%。幸存者的中位随访时间为24年。无病生存率5年时为48%,10至25年保持在45%。除2例复发外,所有复发均发生在最初27个月内。8年后无复发或治疗相关死亡发生。无复发可挽救。除1例初始复发外,所有复发均在腹腔内。在31例行二次探查手术的患者中,84%无肿瘤。二次探查阴性后仅8%的患者复发。分期和术后可触及疾病的存在是重要的预后因素。I期患者5至25年的无病生存率为95%,II期患者5年时为70%,25年时为60%,III期患者5至25年为20%(P < 0.0001)。虽然术后可触及肿瘤的患者无一治愈,但25%存活超过2年。术后无可触及肿瘤的III期患者25年无病生存率为47%。急性毒性可接受,98%的患者完成了放疗。慢性毒性包括12%的小肠梗阻率和3%的致命性第二原发恶性肿瘤/血液学毒性率(2例急性髓细胞白血病,1例血小板减少症)。
随后三十年的多药化疗试验并未超过腹盆腔放疗后单药烷化剂化疗所获得的长期无病生存率。腹部放疗可能有助于巩固多药化疗后的完全缓解,特别是通过调强放疗提高上腹部剂量,并可能与化疗联合使用。
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