Molecular basis for the binding promiscuity of an anti-p24 (HIV-1) monoclonal antibody

被引:158
作者
Kramer, A
Keitel, T
Winkler, K
Stocklein, W
Hohne, W
SchneiderMergener, J
机构
[1] HUMBOLDT UNIV BERLIN,KLINIKUM CHARITE,INST MED IMMUNOL,D-10098 BERLIN,GERMANY
[2] HUMBOLDT UNIV BERLIN,KLINIKUM CHARITE,INST BIOCHEM,D-10098 BERLIN,GERMANY
[3] MAX DELBRUCK CENTRUM,UNIV POTSDAM,INST BIOCHEM & MOL PHYSIOL,D-13122 BERLIN,GERMANY
关键词
D O I
10.1016/S0092-8674(00)80468-7
中图分类号
Q5 [生物化学]; Q7 [分子生物学];
学科分类号
071010 ; 081704 ;
摘要
Multiple binding capabilities utilized by specific protein-to-protein interactions in molecular recognition events are being documented increasingly but remain poorly understood at the molecular level. We identified five unrelated peptides that compete with each other for binding to the paratope region of the monoclonal anti-p24 (HIV-1) antibody CB4-1 by using a synthetic positional scanning combinatorial library XXXX[B-1,B-2,B-3,X-1,X-2,X-3]XXXX (14 mers; 68,590 peptide mixtures in total) prepared by spot synthesis. Complete sets of substitution analogs of the five peptides revealed key interacting residues, information that led to the construction of binding supertopes derived from each peptide. These supertope sequences were identified in hundreds of heterologous proteins, and those proteins that could be obtained were shown to bind CB4-1. Implications of these findings for immune escape mechanisms and autoimmunity are discussed.
引用
收藏
页码:799 / 809
页数:11
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