Structure- and sequence-based design of synthetic single-domain antibody libraries

外域 单域抗体 计算生物学 表位 副镜 肽库 抗体 噬菌体展示 平移(音频) 亲和力成熟 重链 化学 生物 受体 肽序列 生物化学 遗传学 基因 缩放 古生物学 镜头(地质)
作者
Alexander M. Sevy,Ming‐Tang Chen,Michelle E. Castor,Tyler Sylvia,Harini Krishnamurthy,Andrii Ishchenko,Chung-Ming Hsieh
出处
期刊:Protein Engineering Design & Selection [Oxford University Press]
卷期号:33 被引量:22
标识
DOI:10.1093/protein/gzaa028
摘要

Abstract Single-domain antibody fragments known as VHH have emerged in the pharmaceutical industry as useful biotherapeutics. These molecules, which are naturally produced by camelids, share the characteristics of high affinity and specificity with traditional human immunoglobulins, while consisting of only a single heavy chain. Currently, the most common method for generating VHH is via animal immunization, which can be costly and time-consuming. Here we describe the development of a synthetic VHH library for in vitro selection of single domain binders. We combine structure-based design and next-generation sequencing analysis to build a library with characteristics that closely mimic the natural repertoire. To validate the performance of our synthetic library, we isolated VHH against three model antigens (soluble mouse PD-1 ectodomain, amyloid-β peptide, and MrgX1 GPCR) of different sizes and characteristics. We were able to isolate diverse binders targeting different epitopes with high affinity (as high as 5 nM) against all three targets. We then show that anti-mPD-1 binders have functional activity in a receptor blocking assay.
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