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肿瘤特异性抗体介导的主要组织相容性复合体-肽复合物靶向作用可在体内诱导人肿瘤异种移植瘤消退。

Tumor-specific Ab-mediated targeting of MHC-peptide complexes induces regression of human tumor xenografts in vivo.

作者信息

Lev Avital, Noy Roy, Oved Kfir, Novak Hila, Segal Dina, Walden Peter, Zehn Dietmar, Reiter Yoram

机构信息

Faculty of Biology, Technion-Israel Institute of Technology, Haifa 32000, Israel.

出版信息

Proc Natl Acad Sci U S A. 2004 Jun 15;101(24):9051-6. doi: 10.1073/pnas.0403222101. Epub 2004 Jun 7.

Abstract

A cancer immunotherapy strategy is described herein that combines the advantage of the well established tumor targeting capabilities of high-affinity recombinant fragments of Abs with the known efficient, specific, and potent killing ability of CD8 T lymphocytes directed against highly antigenic MHC-peptide complexes. Structurally, it consists of a previously uncharacterized class of recombinant chimerical molecules created by the genetic fusion of single-chain (sc) Fv Ab fragments, specific for tumor cell surface antigens, to monomeric scHLA-A2 complexes containing immunodominant tumor- or viral-specific peptides. The fusion protein can induce very efficiently tumor cell lysis, regardless of the expression of self peptide-MHC complexes. Moreover, these molecules exhibited very potent antitumor activity in vivo in nude mice bearing preestablished human tumor xenografts. These in vitro and in vivo results suggest that recombinant scFv-MHC-peptide fusion molecules could represent an approach to immunotherapy, bridging Ab and T lymphocyte attack on cancer cells.

摘要

本文描述了一种癌症免疫治疗策略,该策略结合了成熟的高亲和力抗体重组片段的肿瘤靶向能力优势与已知的针对高抗原性MHC-肽复合物的CD8 T淋巴细胞高效、特异且强大的杀伤能力。在结构上,它由一类以前未被表征的重组嵌合分子组成,这些分子通过将针对肿瘤细胞表面抗原的单链(sc)Fv抗体片段与含有免疫显性肿瘤或病毒特异性肽的单体scHLA-A2复合物进行基因融合而产生。无论自身肽-MHC复合物的表达情况如何,融合蛋白都能非常有效地诱导肿瘤细胞裂解。此外,这些分子在携带预先建立的人肿瘤异种移植的裸鼠体内表现出非常强大的抗肿瘤活性。这些体外和体内结果表明,重组scFv-MHC-肽融合分子可能代表一种免疫治疗方法,弥合了抗体和T淋巴细胞对癌细胞的攻击。

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