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铋-212标记的抗Tac单克隆抗体:发射α粒子的放射性核素作为放射免疫治疗的手段

Bismuth-212-labeled anti-Tac monoclonal antibody: alpha-particle-emitting radionuclides as modalities for radioimmunotherapy.

作者信息

Kozak R W, Atcher R W, Gansow O A, Friedman A M, Hines J J, Waldmann T A

出版信息

Proc Natl Acad Sci U S A. 1986 Jan;83(2):474-8. doi: 10.1073/pnas.83.2.474.

Abstract

Anti-Tac, a monoclonal antibody directed to the human interleukin 2 (IL-2) receptor, has been successfully conjugated to the alpha-particle-emitting radionuclide bismuth-212 by use of a bifunctional ligand, the isobutylcarboxycarbonic anhydride of diethylenetriaminepentaacetic acid. The physical properties of 212Bi are appropriate for radioimmunotherapy in that it has a short half-life, deposits its high energy over a short distance, and can be obtained in large quantities from a radium generator. Antibody specific activities of 1-40 microCi/microgram (1 Ci = 37 GBq) were achieved. Specificity of the 212Bi-labeled anti-Tac was demonstrated for the IL-2 receptor-positive adult T-cell leukemia line HUT-102B2 by protein synthesis inhibition and clonogenic assays. Activity levels of 0.5 microCi or the equivalent of 12 rad/ml of alpha radiation targeted by anti-Tac eliminated greater than 98% the proliferative capabilities of HUT-102B2 cells with more modest effects on IL-2 receptor-negative cell lines. Specific cytotoxicity was blocked by excess unlabeled anti-Tac but not by human IgG. In addition, an irrelevant control monoclonal antibody of the same isotype labeled with 212Bi was unable to target alpha radiation to cell lines. Therefore, 212Bi-labeled anti-Tac is a potentially effective and specific immunocytotoxic reagent for the elimination of IL-2 receptor-positive cells. These experiments thus provide the scientific basis for use of alpha-particle-emitting radionuclides in immunotherapy.

摘要

抗 Tac 单抗是一种针对人白细胞介素 2(IL-2)受体的单克隆抗体,通过使用双功能配体二乙烯三胺五乙酸异丁基羧基碳酸酐,已成功与发射α粒子的放射性核素铋 -212 偶联。铋 -212 的物理性质适合放射免疫治疗,因为它半衰期短,在短距离内沉积高能量,并且可以从镭发生器大量获得。实现了 1 - 40 微居里/微克(1 居里 = 37 吉贝可)的抗体比活度。通过蛋白质合成抑制和克隆形成试验证明了铋 -212 标记的抗 Tac 对 IL-2 受体阳性的成人 T 细胞白血病细胞系 HUT-102B2 的特异性。抗 Tac 靶向的 0.5 微居里或相当于 12 拉德/毫升α辐射的活性水平消除了 HUT-102B2 细胞大于 98%的增殖能力,对 IL-2 受体阴性细胞系的影响较小。特异性细胞毒性被过量未标记的抗 Tac 阻断,但未被人 IgG 阻断。此外,用铋 -212 标记的相同亚型的无关对照单克隆抗体无法将α辐射靶向细胞系。因此,铋 -212 标记的抗 Tac 是一种潜在有效的特异性免疫细胞毒性试剂,用于消除 IL-2 受体阳性细胞。这些实验从而为在免疫治疗中使用发射α粒子的放射性核素提供了科学依据。

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