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表达针对共享MAGE-A表位的异源性变体筛选出的类似TCR抗体的T细胞不识别同源表位。

T Cells Expressing a TCR-Like Antibody Selected Against the Heteroclitic Variant of a Shared MAGE-A Epitope Do Not Recognise the Cognate Epitope.

作者信息

Saeed Mesha, Schooten Erik, van Brakel Mandy, Cole David K, Ten Hagen Timo L M, Debets Reno

机构信息

Laboratory of Experimental Oncology, Department of Pathology, Erasmus MC, 3000 CA Rotterdam, The Netherlands.

Laboratory of Tumor Immunology, Department of Medical Oncology, Erasmus MC Cancer Institute, 3000 CA Rotterdam, The Netherlands.

出版信息

Cancers (Basel). 2020 May 16;12(5):1255. doi: 10.3390/cancers12051255.

DOI:10.3390/cancers12051255
PMID:32429338
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC7281252/
Abstract

Antibodies-recognising peptides bound to the major histocompatibility complex (pMHC) represent potentially valuable and promising targets for chimeric antigen receptor (CAR) T cells to treat patients with cancer. Here, a human phage-Fab library has been selected using HLA-A2 complexed with a heteroclitic peptide variant from an epitope shared among multiple melanoma-associated antigens (MAGEs). DNA restriction analyses and phage ELISAs confirmed selection of unique antibody clones that specifically bind to HLA-A2 complexes or HLA-A2-positive target cells loaded with native or heteroclitic peptide. Antibodies selected against heteroclitic peptide, in contrast to native peptide, demonstrated significantly lower to even negligible binding towards native peptide or tumour cells that naturally expressed peptides. The binding to native peptide was not rescued by phage panning with antigen-positive tumour cells. Importantly, when antibodies directed against heteroclitic peptides were engineered into CARs and expressed by T cells, binding to native peptides and tumour cells was minimal to absent. In short, TCR-like antibodies, when isolated from a human Fab phage library using heteroclitic peptide, fail to recognise its native peptide. We therefore argue that peptide modifications to improve antibody selections should be performed with caution as resulting antibodies, either used directly or as CARs, may lose activity towards endogenously presented tumour epitopes.

摘要

识别与主要组织相容性复合体结合的肽段(pMHC)的抗体,是嵌合抗原受体(CAR)T细胞治疗癌症患者潜在有价值且前景广阔的靶点。在此,利用与来自多种黑色素瘤相关抗原(MAGE)共有表位的异源性肽变体复合的HLA-A2,筛选了一个人噬菌体-Fab文库。DNA限制性分析和噬菌体ELISA证实,筛选出了能特异性结合HLA-A2复合体或负载天然或异源性肽的HLA-A2阳性靶细胞的独特抗体克隆。与天然肽相比,针对异源性肽筛选出的抗体对天然肽或天然表达肽的肿瘤细胞的结合显著降低甚至可忽略不计。用抗原阳性肿瘤细胞进行噬菌体淘选并不能恢复其与天然肽的结合。重要的是,当将针对异源性肽的抗体构建到CAR中并由T细胞表达时,与天然肽和肿瘤细胞的结合极少甚至不存在。简而言之,当从人Fab噬菌体文库中使用异源性肽分离出类似TCR的抗体时,它们无法识别其天然肽。因此,我们认为,在改善抗体筛选的肽修饰操作时应谨慎,因为由此产生的抗体,无论是直接使用还是作为CAR使用,都可能对内源性呈现的肿瘤表位失去活性。

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J Immunother Cancer. 2017 Mar 21;5:22. doi: 10.1186/s40425-017-0222-9. eCollection 2017.
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The Principles of Engineering Immune Cells to Treat Cancer.工程化免疫细胞治疗癌症的原理。
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