Analysis of CD97 expression and manipulation: antibody treatment but not gene targeting curtails granulocyte migration

Henrike Veninga, Susann Becker, Robert M. Hoek, Manja Wobus, Elke Wandel, Jos van der Kaa, Martin van der Valk, Alex F. de Vos, Hannelore Haase, Bronwyn Owens, Tom van der Poll, René A. W. van Lier, J. Sjef Verbeek, Gabriela Aust, Jörg Hamann

Research output: Contribution to journalArticleAcademicpeer-review

60 Citations (Scopus)

Abstract

The heptahelical receptor CD97 is a defining member of the EGF-TM7 family of adhesion class receptors. In both humans and mice, CD97 isoforms are expressed with variable numbers of tandemly arranged N-terminal epidermal growth factor-like domains that facilitate interactions with distinct cellular ligands. Results from treatment of mice with mAbs in various disease models have suggested a role for CD97 in leukocyte trafficking. Here, we aimed to thoroughly characterize the expression profile of CD97, and delineate its biological function. To this end, we applied a novel polyclonal Ab, which is the first antiserum suitable for immunohistochemistry, and combined this analysis with the study of Cd97-lacZ knock-in mice. We show that similar to the situation in humans, hematopoietic, epithelial, endothelial, muscle, and fat cells expressed CD97. Despite this broad expression pattern, the Cd97(-/-) mouse that we created had no overt phenotype, except for a mild granulocytosis. Furthermore, granulocyte accumulation at sites of inflammation was normal in the absence of CD97. Interestingly, application of CD97 mAbs blocked granulocyte trafficking after thioglycollate-induced peritonitis in wild-type but not in knock-out mice. Hence, we conclude that CD97 mAbs actively induce an inhibitory effect that disturbs normal granulocyte trafficking, which is not perturbed by the absence of the molecule
Original languageEnglish
Pages (from-to)6574-6583
JournalJournal of immunology (Baltimore, Md.
Volume181
Issue number9
DOIs
Publication statusPublished - 2008

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