利妥昔单抗作为惰性非霍奇金淋巴瘤患者的一线及维持治疗药物
Rituximab as first-line and maintenance therapy for patients with indolent non-hodgkin's lymphoma.
作者信息
Hainsworth John D, Litchy Sharlene, Burris Howard A, Scullin Daniel C, Corso Steven W, Yardley Denise A, Morrissey Lisa, Greco F Anthony
机构信息
Sarah Cannon Cancer Center and Tennessee Oncology, Professional Limited Liability Corporation, Nashville, TN, USA.
出版信息
J Clin Oncol. 2002 Oct 15;20(20):4261-7. doi: 10.1200/JCO.2002.08.674.
PURPOSE
To evaluate response to single-agent rituximab in patients with indolent non-Hodgkin's lymphoma (NHL) and no previous systemic therapy, and the feasibility, toxicity, and efficacy of maintenance rituximab, administered at 6-month intervals, in patients with objective response or stable disease after first-line rituximab therapy.
PATIENTS AND METHODS
Patients with indolent NHL (follicular or small lymphocytic subtypes) previously untreated with systemic therapy received rituximab 375 mg/m(2) intravenously weekly for 4 weeks. Patients were restaged at week 6 for response; those with objective response or stable disease received maintenance rituximab courses (identical dose and schedule) at 6-month intervals. Maintenance was continued for a maximum of four rituximab courses or until progression. Between March 1998 and May 1999, 62 patients were entered onto this trial; minimum follow-up was 24 months.
RESULTS
Sixty patients (97%) completed the first 4-week course of rituximab and were assessable for response. All have now completed rituximab therapy; 36 (58%) received four courses at 6-month intervals. The objective response rate at 6 weeks was 47%; 45% of patients had stable disease. With continued maintenance, final response rate increased to 73%, with 37% complete responses. Response was similar in patients with follicular versus small lymphocytic subtypes (76% v 70%, respectively). Median actuarial progression-free survival was 34 months. Two patients experienced grade 3/4 toxicity with the first dose; one patient was removed from treatment. No cumulative or additional toxicities were seen with maintenance courses.
CONCLUSION
Rituximab is highly active and extremely well tolerated as first-line single-agent therapy for indolent NHL. First-line treatment with scheduled maintenance at 6-month intervals produces high overall and complete response rates and a longer progression-free survival (34 months) than has been reported with a standard 4-week treatment.
目的
评估利妥昔单抗单药治疗惰性非霍奇金淋巴瘤(NHL)且既往未接受过全身治疗患者的疗效,以及在一线利妥昔单抗治疗后获得客观缓解或病情稳定的患者中,每6个月给予维持性利妥昔单抗治疗的可行性、毒性和疗效。
患者与方法
既往未接受过全身治疗的惰性NHL(滤泡型或小淋巴细胞型亚型)患者接受利妥昔单抗375mg/m²静脉注射,每周1次,共4周。在第6周对患者进行再次分期以评估疗效;获得客观缓解或病情稳定的患者每6个月接受维持性利妥昔单抗疗程(相同剂量和方案)。维持治疗最多持续4个利妥昔单抗疗程或直至疾病进展。在1998年3月至1999年5月期间,62例患者进入本试验;最短随访时间为24个月。
结果
60例患者(97%)完成了首个4周的利妥昔单抗疗程并可评估疗效。目前所有患者均已完成利妥昔单抗治疗;36例(58%)患者每6个月接受4个疗程的治疗。6周时的客观缓解率为47%;45%的患者病情稳定。随着维持治疗的持续,最终缓解率增至73%,其中37%为完全缓解。滤泡型与小淋巴细胞型亚型患者的缓解情况相似(分别为76%和70%)。中位无进展生存期为34个月。2例患者在首次给药时出现3/4级毒性反应;1例患者停止治疗。维持治疗疗程未观察到累积毒性或额外毒性。
结论
利妥昔单抗作为惰性NHL的一线单药治疗具有高度活性且耐受性极佳。每6个月进行计划性维持的一线治疗可产生较高的总缓解率和完全缓解率,且无进展生存期(34个月)长于标准4周治疗所报告的生存期。
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