P-selectin glycoprotein ligand-1 mediates rolling of human neutrophils on P-selectin.

Kevin L. Moore(University of Oklahoma Health Sciences Center), Kamala D. Patel(University of Oklahoma Health Sciences Center), Richard E. Bruehl(University of Oklahoma Health Sciences Center), Feng Li(University of Oklahoma Health Sciences Center), Douglas A. Johnson(University of Oklahoma Health Sciences Center), Henri S. Lichenstein(University of Oklahoma Health Sciences Center), Richard D. Cummings(University of Oklahoma Health Sciences Center), D F Bainton(University of Oklahoma Health Sciences Center), Rodger P. McEver(University of Oklahoma Health Sciences Center)
The Journal of Cell Biology
February 15, 1995
Cited by 728Open Access
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Abstract

Neutrophils roll on P-selectin expressed by activated platelets or endothelial cells under the shear stresses in the microcirculation. P-selectin glycoprotein ligand-1 (PSGL-1) is a high affinity ligand for P-selectin on myeloid cells. However, it has not been demonstrated that PSGL-1 contributes to the rolling of neutrophils on P-selectin. We developed two IgG mAbs, PL1 and PL2, that appear to recognize protein-dependent epitopes on human PSGL-1. The mAbs bound to PSGL-1 on all leukocytes as well as on heterologous cells transfected with PSGL-1 cDNA. PL1, but not PL2, blocked binding of 125-I-PSGL-1 to immobilized P-selectin, binding of fluid-phase P-selectin to myeloid and lymphoid leukocytes, adhesion of neutrophils to immobilized P-selectin under static conditions, and rolling of neutrophils on P-selectin-expressing CHO cells under a range of shear stresses. PSGL-1 was localized to microvilli on neutrophils, a topography that may facilitate its adhesive function. These data indicate that (a) PSGL-1 accounts for the high affinity binding sites for P-selectin on leukocytes, and (b) PSGL-1 must interact with P-selectin in order for neutrophils to roll on P-selectin at physiological shear stresses.


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