Platelet Glycoprotein Ib: A Zinc-Dependent Binding Protein for the Heavy Chain of High-Molecular-Weight Kininogen

被引:0
作者
Kusumam Joseph
Yoshitaka Nakazawa
Wadie F. Bahou
Berhane Ghebrehiwet
Allen P. Kaplan
机构
[1] Medical University of South Carolina,Department of Medicine, Division of Pulmonary/Critical Care and Allergy/Clinical Immunology
[2] State University of New York,Department of Medicine
来源
Molecular Medicine | 1999年 / 5卷
关键词
High Molecular Weight Kininogen; anti-GPIb Antibody; Glycocalicin; Thrombin Receptor; Platelet Membrane Protein;
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摘要
Domains 3 and 5 of high-molecular-weight kininogen (HK) have been shown to bind to platelets in a zinc-dependent reaction. However, the platelet-binding proteins responsible for this interaction have not been identified. We have focused on the platelet-binding site for the heavy chain (domain 3), which we approached using a domain 3-derived peptide ligand and isolated binding proteins by affinity chromatography. The domain 3-derived peptide, thrombin, HK, factor XII, as well as antibody to glycocalicin (the N-terminal portion of the α chain of GPIb) recognized a protein at 74 kD. We also isolated the thrombin receptor (PAR 1) at 45 kD, however, none of the above-mentioned ligands bound to this protein. Isolation of platelet membrane proteins using a monoclonal anti-glycocalicin antibody column revealed the same HK binding protein at 74 kD, which was reactive with anti-GPIb and represents a GPIb fragment. By photoaffinity labeling, HK interacted with membrane GPIb, which was then isolated in native form (135 kD) along with gC1qR, a ligand for the HK light chain. Finally, 125I-HK binding to platelets was significantly inhibited by the anti-GPIb antibody. These results suggest that the GPIb α chain, a known thrombin binding protein, is also one of the zinc-dependent platelet membrane binding sites for HK domain 3.
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页码:555 / 563
页数:8
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