The Ohio State University, Columbus, OH 43210, USA.
J Clin Oncol. 2010 Oct 10;28(29):4500-6. doi: 10.1200/JCO.2010.29.7978. Epub 2010 Aug 9.
To determine if alemtuzumab consolidation improves response rate and progression-free survival (PFS) after induction chemoimmunotherapy in previously untreated symptomatic patients with chronic lymphocytic leukemia.
Patients (n = 102) received fludarabine 25 mg/m(2) intravenously days 1 to 5 and rituximab 50 mg/m(2) day 1, 325 mg/m(2) day 3, and 375 mg/m(2) day 5 of cycle 1 and then 375 mg/m(2) day 1 of cycles 2 to 6; fludarabine plus rituximab (FR) administration was repeated every 28 days for six cycles. Three months after completion of FR, patients with stable disease or better response received subcutaneous alemtuzumab 3 mg day 1, 10 mg day 3, and 30 mg day 5 and then 30 mg three times per week for 5 weeks.
Overall response (OR), complete response (CR), and partial response (PR) rates were 90%, 29%, and 61% after FR, respectively; 15% of patients were minimal residual disease (MRD) negative. Of 102 patients, 58 received alemtuzumab; 28 (61%) of 46 patients achieving PR after FR attained CR after alemtuzumab. By intent to treat (n = 102), OR and CR rates were 90% and 57% after alemtuzumab, respectively; 42% of patients became MRD negative. With median follow-up of 36 months, median PFS was 36 months, 2-year PFS was 72%, and 2-year OS was 86%. In patients achieving CR after FR, alemtuzumab was associated with five deaths resulting from infection (viral and Listeria meningitis and Legionella, cytomegalovirus, and Pneumocystis pneumonias), which occurred up to 7 months after last therapy. The study was amended to exclude CR patients from receiving alemtuzumab.
Alemtuzumab consolidation improved CR and MRD-negative rates after FR induction but caused serious infections in patients who had already achieved CR after induction and did not improve 2-year PFS or survival.
确定在未经治疗的有症状慢性淋巴细胞白血病患者中,在诱导化疗免疫治疗后使用阿仑单抗巩固治疗是否能提高缓解率和无进展生存期(PFS)。
患者(n=102)接受氟达拉滨 25mg/m²静脉输注第 1 至 5 天和利妥昔单抗 50mg/m²第 1 天、325mg/m²第 3 天和 375mg/m²第 5 天,在第 1 周期的第 32 天和第 6 周期的第 1 天重复给予 375mg/m²氟达拉滨加利妥昔单抗(FR)治疗。在 FR 完成后 3 个月,对病情稳定或有更好反应的患者给予皮下注射阿仑单抗 3mg 第 1 天、10mg 第 3 天和 30mg 第 5 天,然后每周 3 次 30mg 连续 5 周。
FR 后总体缓解(OR)、完全缓解(CR)和部分缓解(PR)率分别为 90%、29%和 61%;15%的患者为微小残留疾病(MRD)阴性。在 102 例患者中,58 例接受了阿仑单抗治疗;在 FR 后达到 PR 的 46 例患者中有 28 例(61%)在接受阿仑单抗后达到了 CR。根据意向治疗(n=102),阿仑单抗后 OR 和 CR 率分别为 90%和 57%;42%的患者成为 MRD 阴性。中位随访 36 个月后,中位 PFS 为 36 个月,2 年 PFS 为 72%,2 年 OS 为 86%。在 FR 后达到 CR 的患者中,阿仑单抗导致 5 例因感染(病毒和李斯特菌脑膜炎和军团菌、巨细胞病毒和卡氏肺孢子虫肺炎)导致的死亡,这些感染发生在最后一次治疗后长达 7 个月。该研究被修订为排除 CR 患者接受阿仑单抗治疗。
阿仑单抗巩固治疗在 FR 诱导后提高了 CR 和 MRD 阴性率,但在诱导后已达到 CR 的患者中引起了严重感染,并未改善 2 年 PFS 或生存率。
