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Robust in vitro affinity maturation strategy based on interface-focused high-throughput mutational scanning

机译:基于面向界面的高通量突变扫描的鲁棒体外亲和力成熟策略

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摘要

Development of protein therapeutics or biosensors often requires in vitro affinity maturation. Here we report a robust affinity engineering strategy using a custom designed library. The strategy consists of two steps beginning with identification of beneficial single amino acid substitutions then combination. A high quality combinatorial library specifically customized to a given binding-interface can be rapidly designed by high-throughput mutational scanning of single substitution libraries. When applied to the optimization of a model antibody Fab fragment, the strategy created a diverse panel of high affinity variants. The most potent variant achieved 2110-fold affinity improvement to an equilibrium dissociation constant (Kd) of 3.45. pM with only 7 amino acid substitutions. The method should facilitate affinity engineering of a wide variety of protein-protein interactions due to its context-dependent library design strategy.
机译:蛋白质治疗剂或生物传感器的开发通常需要体外亲和力成熟。在这里,我们报告了使用自定义设计的库的可靠的相似性工程策略。该策略包括两个步骤,首先是确定有益的单个氨基酸取代,然后进行组合。通过对单个取代文库进行高通量突变扫描,可以快速设计专门针对给定结合界面定制的高质量组合文库。当应用于模型抗体Fab片段的优化时,该策略创建了一组高亲和力变异体。最有效的变体实现了2110倍的亲和力提高,平衡解离常数(Kd)为3.45。仅具有7个氨基酸取代的pM。由于其依赖于上下文的文库设计策略,该方法应有助于各种蛋白质-蛋白质相互作用的亲和力工程。

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