作者
Aaron G Schmidt, Huafeng Xu, Amir R Khan, Timothy O’Donnell, Surender Khurana, Lisa R King, Jody Manischewitz, Hana Golding, Pirada Suphaphiphat, Andrea Carfi, Ethan C Settembre, Philip R Dormitzer, Thomas B Kepler, Ruijun Zhang, M Anthony Moody, Barton F Haynes, Hua-Xin Liao, David E Shaw, Stephen C Harrison
发表日期
2013/1/2
期刊
Proceedings of the National Academy of Sciences
卷号
110
期号
1
页码范围
264-269
出版商
National Academy of Sciences
简介
Affinity maturation refines a naive B-cell response by selecting mutations in antibody variable domains that enhance antigen binding. We describe a B-cell lineage expressing broadly neutralizing influenza virus antibodies derived from a subject immunized with the 2007 trivalent vaccine. The lineage comprises three mature antibodies, the unmutated common ancestor, and a common intermediate. Their heavy-chain complementarity determining region inserts into the conserved receptor-binding pocket of influenza HA. We show by analysis of structures, binding kinetics and long time-scale molecular dynamics simulations that antibody evolution in this lineage has rigidified the initially flexible heavy-chain complementarity determining region by two nearly independent pathways and that this preconfiguration accounts for most of the affinity gain. The results advance our understanding of strategies for developing …
学术搜索中的文章
AG Schmidt, H Xu, AR Khan, T O'Donnell, S Khurana… - Proceedings of the National Academy of Sciences, 2013