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人源单克隆抗体与单克隆抗体的多特异性

Human monoclonal antibodies and monoclonal antibody multispecificity.

作者信息

Campbell A M, Whitford P, Leake R E

机构信息

Department of Biochemistry, University of Glasgow, UK.

出版信息

Br J Cancer. 1987 Dec;56(6):709-13. doi: 10.1038/bjc.1987.275.

Abstract

The majority of human anti-tumour monoclonal antibodies (Mabs) isolated to date have been disappointing. Firstly, they react or cross react with intracellular cytoskeletal proteins or nuclear antigens and therefore are of limited value as blood borne agents. They are also generally of the IgM isotype and show relatively low intrinsic affinity for the primary epitope. Secondly, such Mabs can be generated from normal, non tumour bearing subjects at a frequency comparable to their production from tumour patients. This latter observation is true also for common autoantigens such as DNA and IgG since Mabs to these can also be generated from normal subjects in addition to autoimmune individuals. This article rationalises these observations in the context of the requirement for clinical use for human Mabs. It discusses the evidence that there is a potentially useful B cell response to be immortalised, and examines the consequences of the newly recognised phenomenon of monoclonal antibody multispecificity both on the methodology of their generation and on their subsequent use as imaging and therapeutic tools.

摘要

迄今为止分离出的大多数人抗肿瘤单克隆抗体(Mabs)都不尽人意。首先,它们会与细胞内细胞骨架蛋白或核抗原发生反应或交叉反应,因此作为血源性药物的价值有限。它们通常也是IgM同种型,对主要表位的内在亲和力相对较低。其次,这类单克隆抗体可以从正常的、未患肿瘤的受试者中产生,其频率与从肿瘤患者中产生的频率相当。对于常见的自身抗原,如DNA和IgG,后一种观察结果也是如此,因为除了自身免疫个体外,正常受试者也能产生针对这些抗原的单克隆抗体。本文结合人源单克隆抗体临床应用的要求,对这些观察结果进行了合理的解释。它讨论了存在一种有待永生化的潜在有用B细胞反应的证据,并研究了新认识到的单克隆抗体多特异性现象对其产生方法以及随后作为成像和治疗工具使用的影响。

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