Experimental Transplantation and Immunology Branch, Center for Cancer Research, National Cancer Institute, National Institutes of Health, Bethesda, Maryland 20892, USA.
J Biol Chem. 2012 Aug 17;287(34):28206-14. doi: 10.1074/jbc.M112.384594. Epub 2012 Jul 3.
Bispecific antibodies (biAbs) that mediate cytotoxicity by recruiting and activating endogenous immune cells are an emerging class of next-generation antibody therapeutics. Of particular interest are biAbs of relatively small size (∼50 kDa) that can redirect cytotoxic T cells through simultaneous binding of tumor cells. Here we describe a conceptually unique class of biAbs in which the tumor cell specificity of a humanized antibody fragment that recognizes CD3 on T cells is chemically programmed through a C-terminal selenocysteine (Sec) residue. We demonstrate that through chemically programmed specificity for integrin α(4)β(1) or folate receptor 1 (FOLR1), and common specificity for CD3, these hybrid molecules exert potent and specific in vitro and ex vivo cytotoxicity toward tumor cell lines and primary tumor cells in the presence of primary T cells. Importantly, the generic nature of chemical programming allows one to apply our approach to virtually any specificity, promising a broad utility of chemically programmed biAbs in cancer therapy.
双特异性抗体(biAbs)通过募集和激活内源性免疫细胞来介导细胞毒性,是一类新兴的下一代抗体治疗药物。特别引人关注的是相对较小尺寸(约 50 kDa)的 biAbs,它可以通过同时结合肿瘤细胞来重新定向细胞毒性 T 细胞。在这里,我们描述了一类具有独特概念的 biAbs,其中通过 C 末端硒代半胱氨酸(Sec)残基化学程序化的是识别 T 细胞上 CD3 的人源化抗体片段的肿瘤细胞特异性。我们证明,通过对整合素 α(4)β(1)或叶酸受体 1(FOLR1)的化学程序化特异性以及对 CD3 的共同特异性,这些杂交分子在存在原代 T 细胞的情况下,对肿瘤细胞系和原代肿瘤细胞表现出强大且特异性的体外和离体细胞毒性。重要的是,化学程序化的通用性使得人们可以将我们的方法应用于几乎任何特异性,有望在癌症治疗中广泛应用化学程序化的 biAbs。
