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用于增强激动剂活性的全长IgG形式的靶向TpoR抗体的亲和力成熟。

Affinity maturation of an TpoR targeting antibody in full-length IgG form for enhanced agonist activity.

作者信息

Yang Zhuo, Du Mingjuan, Wang Wei, Xin Xiu, Ma Peixiang, Zhang Hongkai, Lerner Richard A

机构信息

Shanghai Institute for Advanced Immunochemical Studies, ShanghaiTech University, Shanghai, China.

Institute of Biochemistry and Cell Biology, Shanghai Institutes for Biological Sciences, Chinese Academy of Sciences, Shanghai, China.

出版信息

Protein Eng Des Sel. 2018 Jul 1;31(7-8):233-241. doi: 10.1093/protein/gzy002.

Abstract

It has been observed that converting scFv formatted antibodies to full-length IgG often associates with loss of affinity. We aim to address this issue in this paper by establishing an integrated affinity maturation method applying yeast display technology platform. To demonstrate that, we employed a human thrombopoietin receptor targeting antibody named 3D9 which was identified previously from a combinational antibody library in scFv-Fc fusion protein form. We have observed that significant potency loss happened when 3D9 was transformed to full-length IgG form. In this study, we tested whether the potency of the full-length IgG can be improved by affinity maturation of 3D9 using a modified Fab yeast display platform. An efficient CDR3 targeted mutagenesis strategy was designed for Fab library with pre-designed CDR diversity. Next generation sequencing was also used for evaluation of the enrichment process and investigation of sequence-function relationship of the antibody. A variant with improved affinity and higher potency was identified. The study demonstrates that the strategy we used here are efficient for optimizing affinity and activity of full-length IgGs.

摘要

据观察,将单链抗体片段(scFv)形式的抗体转化为全长IgG时,亲和力往往会丧失。在本文中,我们旨在通过建立一种应用酵母展示技术平台的综合亲和力成熟方法来解决这一问题。为了证明这一点,我们使用了一种名为3D9的靶向人血小板生成素受体的抗体,该抗体先前从组合抗体文库中以scFv-Fc融合蛋白形式鉴定得到。我们观察到,当3D9转化为全长IgG形式时,效力显著丧失。在本研究中,我们测试了使用改良的Fab酵母展示平台对3D9进行亲和力成熟是否可以提高全长IgG的效力。针对具有预先设计的互补决定区(CDR)多样性的Fab文库设计了一种有效的靶向CDR3诱变策略。下一代测序也用于评估富集过程和研究抗体的序列-功能关系。鉴定出了一种具有更高亲和力和效力的变体。该研究表明,我们在此使用的策略对于优化全长IgG的亲和力和活性是有效的。

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