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用抗多能K-562干细胞抗体对人类白血病进行免疫治疗。

Immunotherapy of human leukemia with antibody to pluripotential K-562 stem cells.

作者信息

Izquierdo J, Robbio E R, Lozzio B B, Hanna W

出版信息

J Cancer Res Clin Oncol. 1983;105(1):83-93. doi: 10.1007/BF00391837.

Abstract

Gamma (gamma) globulin was fractionated from the serum of a goat immunized with the pluripotential leukemia cell line K-562. The lyophilized gamma-globulin preparation, termed leukoglobulin, contained about 50% immune IgG and suppressed the proliferation of heterotransplanted leukemia and lymphoma cells of human origin. The main aims of this study were to evaluate the potential therapeutic value of leukoglobulin and to determine its toxicity in humans with terminal leukemia and patients whose disease was unresponsive to current therapy. Two patients with CML, one with AMML, four with ALL, and one with AML were treated once a week for up to 5 weeks with leukoglobulin intravenously at doses ranging from 2 to 29 mg/kg. Leukoglobulin was well tolerated with minimal adverse effects and produced an initial mobilization of blasts from the bone marrow, spleen, and other organs with a parallel increase in the number of blasts in the systemic circulation. Subsequent injections of leukoglobulin led to a sharp decrease and the eventual eradication of blasts from the peripheral blood and bone marrow. Except in patients with CML, immature cells other than blasts also markedly diminished. The results of the clinical trials indicated a synergism with or potentiation of most chemotherapeutic agents used. Two possible uses for a combination of leukoglobulin and antileukemic drugs are indicated by the results we report here; drug-antibody synergism for cases showing no response to chemotherapy alone or leukoglobulin given immediately after chemotherapy is administered to eliminate residual leukemia cells. Alternatively, leukoglobulin can be given as a single therapeutic agent during the induction or maintenance phases of treatment to patients with leukemia resistant to other therapeutic combinations.

摘要

从用多能白血病细胞系K - 562免疫的山羊血清中分离出γ球蛋白。冻干的γ球蛋白制剂称为白细胞球蛋白,含有约50%的免疫IgG,可抑制人源异种移植白血病和淋巴瘤细胞的增殖。本研究的主要目的是评估白细胞球蛋白的潜在治疗价值,并确定其对晚期白血病患者和对当前治疗无反应的患者的毒性。2例慢性粒细胞白血病患者、1例急性粒单核细胞白血病患者、4例急性淋巴细胞白血病患者和1例急性髓细胞白血病患者,每周静脉注射白细胞球蛋白1次,持续5周,剂量范围为2至29mg/kg。白细胞球蛋白耐受性良好,不良反应极小,最初可使骨髓、脾脏和其他器官中的原始细胞动员,同时全身循环中的原始细胞数量平行增加。随后注射白细胞球蛋白导致外周血和骨髓中的原始细胞急剧减少并最终消除。除慢性粒细胞白血病患者外,除原始细胞外的未成熟细胞也明显减少。临床试验结果表明,白细胞球蛋白与大多数使用的化疗药物具有协同作用或增效作用。我们在此报告的结果表明了白细胞球蛋白与抗白血病药物联合使用的两种可能用途;对于单独化疗无反应的病例,药物 - 抗体协同作用,或在化疗后立即给予白细胞球蛋白以消除残留的白血病细胞。或者,对于对其他治疗组合耐药的白血病患者,可在治疗的诱导或维持阶段将白细胞球蛋白作为单一治疗药物使用。

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