Shielding of the A1 domain by the D′D3 domains of von Willebrand factor modulates its interaction with platelet glycoprotein Ib-IX-V

Abstract

Soluble von Willebrand factor (VWF) has a low affinity for platelet glycoprotein (GP) Ibα and needs immobilization and/or high shear stress to enable binding of its A1 domain to the receptor. The previously described anti-VWF monoclonal antibody 1C1E7 enhances VWF/GPIbα binding and recognizes an epitope in the amino acids 764-1035 region in the N-terminal D′D3 domains. In this study we demonstrated that the D′D3 region negatively modulates the VWF/GPIb-IX-V interaction; (i) deletion of the D′D3 region in VWF augmented binding to GPIbα, suggesting an inhibitory role for this region, (ii) the isolated D′D3 region inhibited the GPIbα interaction of a VWF deletion mutant lacking this region, indicating that intramolecular interactions limit the accessibility of the A1 domain, (iii) using a panel of anti-VWF monoclonal antibodies, we next showed that the D′D3 region is in close proximity with the A1 domain in soluble VWF but not when VWF was immobilized; (iv) destroying the epitope of 1C1E7 resulted in a mutant VWF with an increased affinity for GPIbα. Our results support a model of domain translocation in VWF that allows interaction with GPIbα. The suggested shielding interaction of the A1 domain by the D′D3 region then becomes disrupted by VWF immobilization. © 2006 by The American Society for Biochemistry and Molecular Biology, Inc.