Monoclonal antibodies (mAb) have great potential value for in vivo diagnosis and therapy in humans. Their antigenic nature is however responsible for severe side effects and successful applications in the clinic have prove to be more limited than was originally hoped. This review summarize both cell biology and molecular biology approaches developed in order to overcome these limitations. Improving methodologies to immortalize cell lines producing human mAbs are reported with a particular attention to the techniques aimed at rescuing B cells expressing high-affinity human antibodies. A major part of this review is devoted to the protein engineering work. Genetic manipulation of mouse monoclonals to produce humanized antibodies and preparation of bacteriophage libraries displaying Ig repertoires are examined. The possibility to extend these approaches to the production of in vitro repertoires and to obviate the in vivo immunization step is also discussed.
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机译:单克隆抗体(mAb)在人体体内诊断和治疗中具有巨大的潜在价值。然而,它们的抗原性质是造成严重副作用的原因,临床上的成功应用被证明比最初希望的要有限。本文总结了为克服这些局限性而开发的细胞生物学和分子生物学方法。报道了改进生产人单克隆抗体的细胞系永生化的方法,特别关注旨在挽救表达高亲和力人类抗体的 B 细胞的技术。本综述的主要部分致力于蛋白质工程工作。研究了小鼠单克隆抗体的遗传操作以产生人源化抗体和制备显示 Ig 组库的噬菌体文库。还讨论了将这些方法扩展到体外库的生产和避免体内免疫步骤的可能性。
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