BACKGROUND AND OBJECTIVES:Alemtuzumab may be effective in Sézary syndrome (SS), an aggressive cutaneous T-cell lymphoma, but is associated with severe hematologic toxicity and infections. This study investigated whether low-dose subcutaneous alemtuzumab can induce hematologic, immunologic, and clinical responses similar to those obtained with the standard regimen, but with less toxicity. DESIGN AND METHODS:Fourteen SS patients were enrolled: 11 had relapsed/refractory disease and three had untreated SS with high counts of circulating Sézary cells (SC). Four received 3 mg alemtuzumab on day 1, 10 mg on day 3, then 15 mg on alternating days; circulating SC were evaluated after the fourth 15 mg dose and treatment was interrupted in the presence of counts <1,000/mm (3). A reduced dosage (3 mg on day 1, then 10 mg on alternating days) was administered to the remaining patients, with SC counted before every injection, until a reduction to values of <1,000/mm (3). RESULTS:The median SC count decreased by 95.5%. Overall, 12/14 patients (85.7%) achieved a clinical response, with three complete responses (21.4%). After a median follow-up of 16 months, the median time-to-treatment failure is 12 months. Infectious complications occurred in 28.6% of patients, all included in the group treated with 15 mg. No patient in the group treated with 10 mg developed hematologic toxicity or infections. An early recovery of circulating NK, B and CD3+CD8+ cells occurred after the first cycle. INTERPRETATION AND CONCLUSIONS:Subcutaneous alemtuzumab at very low doses (10 mg maximum per administration), given for a short period based on SC levels, has a good toxicity profile, high response rate and causes durable remissions in SS patients with high tumor burden in the peripheral blood.

译文

背景与目的:Alemtuzumab可能对Sézary综合征(SS),侵袭性皮肤T细胞淋巴瘤有效,但与严重的血液学毒性和感染有关。这项研究调查了低剂量皮下注射alemtuzumab是否可以诱导血液学,免疫学和临床反应,与标准治疗方案相似,但毒性较小。
设计与方法:招募了14例SS患者:11例复发/难治性疾病和3例未经治疗的SS,其循环中的Sézary细胞(SC)数量高。四名患者在第1天接受3 mg阿仑珠单抗,在第3天接受10 mg,然后每隔一天接受15 mg;在第四个15 mg剂量后评估循环SC,并在计数<1,000 / mm的情况下中断治疗(3)。其余患者服用减少剂量的药物(第1天为3 mg,隔天则为10 mg),每次注射前都要对SC进行计数,直至降至<1,000 / mm(3)。
结果:中位SC计数下降了95.5%。总体而言,有12/14例患者(85.7%)达到了临床缓解,其中3例完全缓解(21.4%)。中位随访16个月后,中位治疗失败时间为12个月。感染并发症发生在28.6%的患者中,所有患者均接受15 mg治疗。用10 mg治疗的组中没有患者出现血液学毒性或感染。在第一个周期后,循环的NK,B和CD3 CD8细胞得以早期恢复。
解释和结论:根据SC水平在短期内给予非常低剂量的皮下注射alemtuzumab(每次给药最大10 mg),具有良好的毒性特征,高响应率,并导致具有高肿瘤负担的SS患者持久缓解。外周血。

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