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具有单价飞摩尔抗原结合亲和力的抗体片段的定向进化。

Directed evolution of antibody fragments with monovalent femtomolar antigen-binding affinity.

作者信息

Boder E T, Midelfort K S, Wittrup K D

机构信息

Department of Chemical Engineering, University of Illinois, Urbana, IL 61801, USA.

出版信息

Proc Natl Acad Sci U S A. 2000 Sep 26;97(20):10701-5. doi: 10.1073/pnas.170297297.

Abstract

Single-chain antibody mutants have been evolved in vitro with antigen-binding equilibrium dissociation constant K(d) = 48 fM and slower dissociation kinetics (half-time > 5 days) than those for the streptavidin-biotin complex. These mutants possess the highest monovalent ligand-binding affinity yet reported for an engineered protein by over two orders of magnitude. Optimal kinetic screening of randomly mutagenized libraries of 10(5)-10(7) yeast surface-displayed antibodies enabled a >1,000-fold decrease in the rate of dissociation after four cycles of affinity mutagenesis and screening. The consensus mutations are generally nonconservative by comparison with naturally occurring mouse Fv sequences and with residues that do not contact the fluorescein antigen in the wild-type complex. The existence of these mutants demonstrates that the antibody Fv architecture is not intrinsically responsible for an antigen-binding affinity ceiling during in vivo affinity maturation.

摘要

单链抗体突变体已在体外进化,其抗原结合平衡解离常数K(d)=48飞摩尔,解离动力学比链霉亲和素-生物素复合物慢(半衰期>5天)。这些突变体具有迄今报道的工程蛋白中最高的单价配体结合亲和力,超过两个数量级。对10(5)-10(7)个酵母表面展示抗体的随机诱变文库进行最佳动力学筛选,在四轮亲和力诱变和筛选后,解离速率降低了1000倍以上。与天然存在的小鼠Fv序列以及野生型复合物中不与荧光素抗原接触的残基相比,共有突变通常是非保守的。这些突变体的存在表明,抗体Fv结构在体内亲和力成熟过程中并非抗原结合亲和力上限的内在原因。

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