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抗体介导的将共价连接的肽靶向人单链I类主要组织相容性复合体可诱导肿瘤或病毒特异性细胞毒性T淋巴细胞有效杀伤肿瘤细胞。

Antibody-mediated targeting of human single-chain class I MHC with covalently linked peptides induces efficient killing of tumor cells by tumor or viral-specific cytotoxic T lymphocytes.

作者信息

Oved Kfir, Lev Avital, Noy Roy, Segal Dina, Reiter Yoram

机构信息

Department of Biology, The Technion-Israel Institute of Technology, Technion City, Room 333, Haifa, 32000, Israel.

出版信息

Cancer Immunol Immunother. 2005 Sep;54(9):867-79. doi: 10.1007/s00262-005-0666-5. Epub 2005 May 20.

Abstract

Soluble forms of human MHC class I HLA-A2 were produced in which the peptide binding groove was uniformly occupied by a single tumor or viral-derived peptides attached via a covalent flexible peptide linker to the N terminus of a single-chain beta-2-microglobulin-HLA-A2 heavy chain fusion protein. A tetravalent version of this molecule with various peptides was found to be functional. It could stimulate T cells specifically as well as bind them with high avidity. The covalently linked single chain peptide-HLA-A2 construct was next fused at its C-terminal end to a scFv antibody fragment derived from the variable domains of an anti-IL-2R alpha subunit-specific humanized antibody, anti-Tac. The scFv-MHC fusion was thus encoded by a single gene and produced in E. coli as a single polypeptide chain. Binding studies revealed its ability to decorate Ag-positive human tumor cells with covalent peptide single-chain HLA-A2 (scHLA-A2) molecules in a manner that was entirely dependent upon the specificity of the targeting Antibody fragment. Most importantly, the covalent scHLA-A2 molecule, when bound to the target tumor cells, could induce efficient and specific HLA-A2-restricted, peptide-specific CTL-mediated lysis. These results demonstrate the ability to generate soluble, stable, and functional single-chain HLA-A2 molecules with covalently linked peptides, which when fused to targeting antibodies, potentiate CTL killing. This new approach may open the way for the development of new immunotherapeutic strategies based on antibody targeting of natural cognate MHC ligands and CTL-based cytotoxic mechanisms.

摘要

产生了人 MHC I 类 HLA - A2 的可溶性形式,其中肽结合槽被单个肿瘤或病毒衍生肽均匀占据,这些肽通过共价柔性肽接头连接到单链β2 - 微球蛋白 - HLA - A2 重链融合蛋白的 N 端。发现这种带有各种肽的分子的四价形式具有功能。它可以特异性刺激 T 细胞,并以高亲和力结合它们。接下来,将共价连接的单链肽 - HLA - A2 构建体在其 C 末端与源自抗 IL - 2Rα亚基特异性人源化抗体 anti - Tac 的可变域的 scFv 抗体片段融合。因此,scFv - MHC 融合体由单个基因编码,并在大肠杆菌中作为单条多肽链产生。结合研究表明,它能够以完全依赖于靶向抗体片段特异性的方式,用共价肽单链 HLA - A2(scHLA - A2)分子修饰 Ag 阳性人肿瘤细胞。最重要的是,共价 scHLA - A2 分子与靶肿瘤细胞结合时,可诱导高效且特异性的 HLA - A2 限制的、肽特异性的 CTL 介导的裂解。这些结果证明了产生具有共价连接肽的可溶性、稳定且功能性单链 HLA - A2 分子的能力,当与靶向抗体融合时,可增强 CTL 杀伤作用。这种新方法可能为基于天然同源 MHC 配体的抗体靶向和基于 CTL 的细胞毒性机制开发新的免疫治疗策略开辟道路。

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