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核糖体展示技术能够有效地在体外从免疫文库中筛选和进化出高亲和力抗体。

Ribosome display efficiently selects and evolves high-affinity antibodies in vitro from immune libraries.

作者信息

Hanes J, Jermutus L, Weber-Bornhauser S, Bosshard H R, Plückthun A

机构信息

Biochemisches Institut, Universität Zürich, Winterthurerstrasse 190, CH-8057 Zürich, Switzerland.

出版信息

Proc Natl Acad Sci U S A. 1998 Nov 24;95(24):14130-5. doi: 10.1073/pnas.95.24.14130.

Abstract

Ribosome display was applied for affinity selection of antibody single-chain fragments (scFv) from a diverse library generated from mice immunized with a variant peptide of the transcription factor GCN4 dimerization domain. After three rounds of ribosome display, positive scFvs were isolated and characterized. Several different scFvs were selected, but those in the largest group were closely related to each other and differed in 0 to 5 amino acid residues with respect to their consensus sequence, the likely common progenitor. The best scFv had a dissociation constant of (4 +/- 1) x 10(-11) M, measured in solution. One amino acid residue in complementarity determining region L1 was found to be responsible for a 65-fold higher affinity than the likely progenitor. It appears that this high-affinity scFv was selected from the mutations occurring during ribosome display in vitro, and that this constitutes an affinity maturation inherent in this method. The in vitro-selected scFvs could be functionally expressed in the Escherichia coli periplasm with good yields or prepared by in vitro refolding. Thus, ribosome display can be a powerful methodology for in vitro library screening and simultaneous sequence evolution.

摘要

核糖体展示技术被应用于从用转录因子GCN4二聚化结构域的变体肽免疫的小鼠产生的多样化文库中亲和选择抗体单链片段(scFv)。经过三轮核糖体展示,分离并鉴定了阳性scFv。选择了几种不同的scFv,但最大组中的那些彼此密切相关,相对于它们可能的共同祖先共有序列,其氨基酸残基有0至5个不同。最佳scFv在溶液中测得的解离常数为(4±1)×10⁻¹¹ M。发现互补决定区L1中的一个氨基酸残基导致其亲和力比可能的祖先高65倍。似乎这种高亲和力scFv是从体外核糖体展示过程中发生的突变中选择出来的,这构成了该方法固有的亲和力成熟。体外选择的scFv可以在大肠杆菌周质中高效功能性表达或通过体外重折叠制备。因此,核糖体展示可以成为体外文库筛选和同时进行序列进化的强大方法。

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