Intercellular adhesion molecule-4 binds α4β1 and αV-family integrins through novel integrin-binding mechanisms

Author:

Spring Frances A.1,Parsons Stephen F.1,Ortlepp Susan1,Olsson Martin L.1,Sessions Richard1,Brady R. Leo1,Anstee David J.1

Affiliation:

1. From the Bristol Institute for Transfusion Sciences; Celltech, Slough; and the University of Bristol, United Kingdom; and the University Hospital Blood Centre, Lund, Sweden.

Abstract

The LW blood group glycoprotein, ICAM-4, is a member of the intercellular adhesion molecule (ICAM) family expressed in erythroid cells. To begin to address the function of this molecule, ligands for ICAM-4 on hemopoietic and nonhemopoietic cell lines were identified. Peptide inhibition studies suggest that adhesion of cell lines to an ICAM-4–Fc construct is mediated by an LDV-inhibitable integrin on hemopoietic cells and an RGD-inhibitable integrin on nonhemopoietic cells. Antibody inhibition studies identified the hemopoietic integrin as α4β1. Antibody inhibition studies on α4β1-negative, nonhemopoietic cell lines suggested that adhesion of these cells is mediated by αVintegrins (notably αVβ1 and αVβ5). The structure of ICAM-4 modeled on the crystal structure of ICAM-2 was used to identify surface-exposed amino acid residues for site-directed mutagenesis. Neither an unusual LETS nor an LDV motif in the first domain of ICAM-4 was critical for integrin binding. ICAM-4 is the first ICAM family member shown to be a ligand for integrins other than those of the β2family, and the data suggest that ICAM-4 has a novel integrin-binding site(s). These findings suggest a role for ICAM-4 in normal erythropoiesis and may also be relevant to the adhesive interactions of sickle cells.

Publisher

American Society of Hematology

Subject

Cell Biology,Hematology,Immunology,Biochemistry

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