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人B细胞淋巴瘤的单克隆抗体1F5(抗CD20)血清疗法。

Monoclonal antibody 1F5 (anti-CD20) serotherapy of human B cell lymphomas.

作者信息

Press O W, Appelbaum F, Ledbetter J A, Martin P J, Zarling J, Kidd P, Thomas E D

出版信息

Blood. 1987 Feb;69(2):584-91.

PMID:3492224
Abstract

Four patients with refractory malignant B cell lymphomas were treated with continuous intravenous (IV) infusions of murine monoclonal antibody (MoAb) 1F5 (anti-CD20) over five to ten days. Dose-dependent levels of free serum 1F5 were detected in all patients. Two patients had circulating tumor cells and in both cases 90% of malignant cells were eliminated from the blood stream within four hours of initiation of serotherapy. Antigenic modulation did not occur, and sustained reduction of circulating tumor cells was observed throughout the duration of the infusions. Serial bone marrow aspirations and lymph node biopsies were examined by immunoperoxidase and immunofluorescence techniques to ascertain MoAb penetration into extravascular sites. High doses (100 to 800 mg/m2/d and high serum 1F5 levels (13 to 190 micrograms/mL) were required to coat tumor cells in these compartments in contrast to the low doses that were adequate for depletion of circulating cells. Clinical response appeared to correlate with dose of MoAb administered with progressive disease (52 mg), stable disease (104 mg), minor response (1,032 mg), and partial response (2,380 mg) observed in consecutive patients. The patient treated with the highest 1F5 dose achieved a 90% reduction in evaluable lymph node disease, but the duration of this remission was brief (six weeks). This study demonstrates that high doses of 1F5 can be administered to patients with negligible toxicity by continuous infusion and that clinical responses can be obtained in patients given greater than 1 g of unmodified antibody over a ten-day period.

摘要

四名难治性恶性B细胞淋巴瘤患者接受了为期五至十天的鼠单克隆抗体(MoAb)1F5(抗CD20)持续静脉输注治疗。所有患者均检测到剂量依赖性的游离血清1F5水平。两名患者有循环肿瘤细胞,在血清疗法开始后的四小时内,这两名患者血液中的恶性细胞均有90%被清除。未发生抗原调制现象,且在输注期间均观察到循环肿瘤细胞持续减少。通过免疫过氧化物酶和免疫荧光技术对系列骨髓穿刺物和淋巴结活检样本进行检查,以确定MoAb渗入血管外部位的情况。与清除循环细胞所需的低剂量相比,需要高剂量(100至800 mg/m²/d)和高血清1F5水平(13至190μg/mL)才能覆盖这些部位的肿瘤细胞。临床反应似乎与给予的MoAb剂量相关,连续患者中观察到疾病进展(52 mg)、病情稳定(104 mg)、轻微反应(1032 mg)和部分反应(2380 mg)。接受最高1F5剂量治疗的患者可评估的淋巴结疾病减少了90%,但缓解期较短(六周)。本研究表明,通过持续输注可向患者给予高剂量的1F5,毒性可忽略不计,且在十天内给予超过1 g未修饰抗体的患者可获得临床反应。

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