Antibody CDR amino acids underlying the functionality of antibody repertoires in recognizing diverse protein antigens

Author:

Peng Hung-Pin,Hsu Hung-Ju,Yu Chung-Ming,Hung Fei-Hung,Tung Chao-Ping,Huang Yu-Chuan,Chen Chi-Yung,Tsai Pei-Hsun,Yang An-Suei

Abstract

AbstractAntibodies recognize protein antigens with exquisite specificity in a complex aqueous environment, where interfacial waters are an integral part of the antibody–protein complex interfaces. In this work, we elucidate, with computational analyses, the principles governing the antibodies’ specificity and affinity towards their cognate protein antigens in the presence of explicit interfacial waters. Experimentally, in four model antibody–protein complexes, we compared the contributions of the interaction types in antibody–protein antigen complex interfaces with the antibody variants selected from phage-displayed synthetic antibody libraries. Evidently, the specific interactions involving a subset of aromatic CDR (complementarity determining region) residues largely form the predominant determinant underlying the specificity of the antibody–protein complexes in nature. The interfacial direct/water-mediated hydrogen bonds accompanying the CDR aromatic interactions are optimized locally but contribute little in determining the epitope location. The results provide insights into the phenomenon that natural antibodies with limited sequence and structural variations in an antibody repertoire can recognize seemingly unlimited protein antigens. Our work suggests guidelines in designing functional artificial antibody repertoires with practical applications in developing novel antibody-based therapeutics and diagnostics for treating and preventing human diseases.

Funder

Academia Sinica

Publisher

Springer Science and Business Media LLC

Subject

Multidisciplinary

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