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通过噬菌体展示技术鉴定靶向肿瘤细胞表面抗原的新型抗体

Identification of New Antibodies Targeting Tumor Cell Surface Antigens by Phage Display.

作者信息

Krohn Steffen, Peipp Matthias, Klausz Katja

机构信息

Division of Antibody-Based Immunotherapy, Department of Internal Medicine II, University Medical Center Schleswig-Holstein and Christian-Albrechts-University Kiel, Kiel, Germany.

出版信息

Methods Mol Biol. 2023;2681:61-82. doi: 10.1007/978-1-0716-3279-6_5.

Abstract

The majority of therapeutic antibodies, bispecific antibodies, and chimeric antigen receptor (CAR) T cells in cancer therapy are based on an antibody or antibody fragment that specifically binds a target present on the surface of a tumor cell. Suitable antigens that can be used for immunotherapy are ideally tumor-specific or tumor-associated and stably expressed on the tumor cell. The identification of new target structures to further optimize immunotherapies could be realized by comparing healthy and tumor cells using "omics" methods to select promising proteins. However, differences in post-translational modifications and structural alterations that can be present on the tumor cell surface are difficult to identify or even not accessible by these techniques. In this chapter, we describe an alternative approach to potentially identify antibodies targeting novel tumor-associated antigens (TAA) or epitopes by using cellular screening and phage display of antibody libraries. Isolated antibody fragments can be further converted into chimeric IgG or other antibody formats to investigate the anti-tumor effector functions and finally identify and characterize the respective antigen.

摘要

癌症治疗中的大多数治疗性抗体、双特异性抗体和嵌合抗原受体(CAR)T细胞都是基于特异性结合肿瘤细胞表面存在的靶标的抗体或抗体片段。可用于免疫治疗的合适抗原理想情况下是肿瘤特异性或肿瘤相关的,并在肿瘤细胞上稳定表达。通过使用“组学”方法比较健康细胞和肿瘤细胞以选择有前景的蛋白质,可实现对新靶标结构的鉴定,从而进一步优化免疫治疗。然而,肿瘤细胞表面可能存在的翻译后修饰和结构改变的差异很难通过这些技术鉴定,甚至无法检测到。在本章中,我们描述了一种替代方法,通过使用细胞筛选和抗体文库的噬菌体展示来潜在地鉴定靶向新型肿瘤相关抗原(TAA)或表位的抗体。分离的抗体片段可进一步转化为嵌合IgG或其他抗体形式,以研究抗肿瘤效应功能,并最终鉴定和表征相应的抗原。

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