CRYSTAL-STRUCTURE OF A HUMAN RHINOVIRUS NEUTRALIZING ANTIBODY COMPLEXED WITH A PEPTIDE DERIVED FROM VIRAL CAPSID PROTEIN VP2

被引:93
作者
TORMO, J
BLAAS, D
PARRY, NR
ROWLANDS, D
STUART, D
FITA, I
机构
[1] ESCOLA TECN SUPER ENGN IND, DEPT ENGN QUIM, E-08028 BARCELONA, SPAIN
[2] UNIV VIENNA, INST BIOCHEM, A-1090 VIENNA, AUSTRIA
[3] WELLCOME RES LABS, DEPT MOLEC SCI, BECKENHAM BR3 3BS, KENT, ENGLAND
[4] UNIV OXFORD, MOLEC BIOPHYS LAB, OXFORD OX1 3QU, ENGLAND
关键词
ANTIBODY STRUCTURE; CROSS-REACTIVITY; CRYSTAL STRUCTURE; HUMAN RHINOVIRUS; VIRAL NEUTRALIZATION;
D O I
10.1002/j.1460-2075.1994.tb06506.x
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
The three-dimensional structure of the complex between the Fab fragment of an anti-human rhinovirus neutralizing antibody (8F5) and a cross-reactive synthetic peptide from the viral capsid protein VP2 has been determined at 2.5 Angstrom resolution by crystallographic methods. The refinement is presently at an R factor of 0.18 and the antigen-binding site and viral peptide are well defined. The peptide antigen adopts a compact fold by two tight turns and interacts through hydrogen bonds, some with ionic character, and van der Waals contacts with antibody residues from the six hypervariable loops as well as several framework amino acids. The conformation adopted by the peptide is closely related to the corresponding region of the viral protein VP2 on the surface of human rhinovirus 1A whose three-dimensional structure is known. Implications for the cross-reactivity between peptides and the viral capsid are discussed. The peptide-antibody interactions, together with the analysis of mutant viruses that escape neutralization by 8F5 suggest two different mechanisms for viral escape. The comparison between the complexed and uncomplexed antibody structures shows important conformational rearrangements, especially in the hypervariable loops of the heavy chain. Thus, it constitutes a clear example of the 'induced fit' molecular recognition mechanism.
引用
收藏
页码:2247 / 2256
页数:10
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