Komaki R, Wadler S, Peters T, Byhardt R W, Order S, Gallagher M J, Herskovic A, Pederson J
Department of Clinical Radiotherapy, University of Texas M. D. Anderson Cancer Center, Houston 77030.
Cancer. 1992 Jun 1;69(11):2807-12. doi: 10.1002/1097-0142(19920601)69:11<2807::aid-cncr2820691128>3.0.co;2-o.
Adenocarcinoma of the pancreas is an extremely malignant neoplasm with a particular propensity to spread to the liver. In an effort to combine chemotherapy with high-dose local irradiation plus a modest dose of irradiation to suspected (subclinical) hepatic metastasis, patients with unresectable pancreatic carcinomas with no known distant metastasis were treated on a prospective multi-institutional Radiation Therapy Oncology Group (RTOG) Phase I/II trial. High total dose continuous radiation therapy to the pancreas (6120 cGy in 34 fractions over 7 weeks) and simultaneous prophylactic hepatic irradiation (PHI, 2340 cGy in 13 fractions for the last 2.5 weeks) were combined with administration of 5-fluorouracil 1000 mg/m2/day (maximum, 1500 mg) by intravenous continuous infusion for 5 days starting on day 1 and repeated on day 30 for 5 days, followed by a dose of 600 mg/m2 as a weekly bolus injection starting during week 9 for 6 months. In 18 months, 81 patients were enrolled in the study; 79 were evaluable with a minimum potential follow-up of 8.2 months. The patients ranged in age from 32 to 75 years (median, 64 years). Karnofsky performance status was 80 to 100 in 74% of patients. The tumor was confined to the head of the pancreas in 72% of patients. The planned radiation therapy for the pancreas was completed in 87% of patients, 80% received the planned PHI, and 85% completed the first two cycles of chemotherapy. Seventy-five percent of patients completed both treatments according to the protocol. Most patients who did not complete both treatments had tumor progression or refused additional therapy. During all cycles of chemotherapy and radiation therapy, 2 patients died of complications (Grade 5, 1 hepatic and 1 infection), 9 had life-threatening reactions (Grade 4, 7 hematologic, 1 neurologic, and 1 mucositis), and 31 patients had severe effects (Grade 3) according to the RTOG toxicity scale. Overall hepatic metastasis was documented in 32% (13% as the first site of failure), persistent or progressive pancreatic tumor was evident in 73%, and abdominal and extra-abdominal spread were reported in 27% and 8% of patients, respectively. Eighty percent (63 patients) died (median survival, 8.4 months). Although this study suggests that PHI may reduce the frequency of hepatic metastasis, failure to control the primary tumor and intraabdominal spread remain overwhelming.
胰腺癌是一种极具恶性的肿瘤,特别容易扩散至肝脏。为了将化疗与高剂量局部照射以及对疑似(亚临床)肝转移灶的适度剂量照射相结合,对无已知远处转移的不可切除胰腺癌患者进行了一项前瞻性多机构放射治疗肿瘤学组(RTOG)I/II期试验。对胰腺进行高总剂量连续放疗(7周内34次分割,共6120 cGy),同时进行预防性肝照射(PHI,在最后2.5周内13次分割,共2340 cGy),并从第1天开始静脉持续输注5-氟尿嘧啶1000 mg/m²/天(最大剂量1500 mg)共5天,第30天重复5天,然后从第9周开始每周推注一次600 mg/m²,持续6个月。在18个月内,81例患者入组该研究;79例可评估,最短潜在随访时间为8.2个月。患者年龄在32至75岁之间(中位年龄64岁)。74%的患者卡氏功能状态评分为80至100。72%的患者肿瘤局限于胰头。87%的患者完成了胰腺的计划放疗,80%的患者接受了计划的PHI,85%的患者完成了前两个化疗周期。75%的患者按照方案完成了两种治疗。大多数未完成两种治疗患者出现肿瘤进展或拒绝进一步治疗。在所有化疗和放疗周期中,2例患者死于并发症(5级,1例肝脏相关,1例感染),9例出现危及生命的反应(4级,7例血液学相关,1例神经学相关,1例黏膜炎),31例患者根据RTOG毒性量表出现严重不良反应(3级)。32%的患者记录有总体肝转移(13%为首个失败部位),73%的患者有持续或进展性胰腺肿瘤,27%和8%的患者分别报告有腹部和腹部外扩散。80%(63例)患者死亡(中位生存期8.4个月)。虽然该研究表明PHI可能降低肝转移频率,但未能控制原发肿瘤和腹腔内扩散仍然是主要问题。
