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Unraveling the Allosteric Mechanism of Serine Protease Inhibition by an Antibody

Overview
Journal Structure
Publisher Cell Press
Specialties Biochemistry
Biotechnology
Cell Biology
Molecular Biology
Date 2009 Dec 17
PMID 20004165
Citations 28
Authors
Rajkumar Ganesan
Charles Eigenbrot
Yan Wu
Wei-Ching Liang
Steven Shia
Michael T Lipari
Daniel Kirchhofer
Affiliations
Soon will be listed here.
Abstract

Recent structural studies have outlined the mechanism of protease inhibition by active site-directed antibodies. However, the molecular basis of allosteric inhibition by antibodies has been elusive. Here we report the 2.35 A resolution structure of the trypsin-like serine protease hepatocyte growth factor activator (HGFA) in complex with the allosteric antibody Ab40, a potent inhibitor of HGFA catalytic activity. The antibody binds at the periphery of the substrate binding cleft and imposes a conformational change on the entire 99-loop (chymotrypsinogen numbering). The altered conformation of the 99-loop is incompatible with substrate binding due to the partial collapse of subsite S2 and the reorganization of subsite S4. Remarkably, a single residue deletion of Ab40 abolished inhibition of HGFA activity, commensurate with the reversal of the 99-loop conformation to its "competent" state. The results define an "allosteric switch" mechanism as the basis of protease inhibition by an allosteric antibody.

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