E- and P-selectin are inducible cell adhesion molecules on endothelial cells, which function as Ca(2+)-dependent lectins and mediate the binding of neutrophils and monocytes. We have recently identified a 150-kD glycoprotein ligand for E-selectin on mouse myeloid cells, using a recombinant antibody-like form of mouse E-selectin. Here, we report that this ligand does not bind to an analogous P-selectin fusion protein. Instead, the chimeric P-selectin-IgG protein recognizes a 160-kD glycoprotein on the mouse neutrophil progenitor 32D cl 3, on mature mouse neutrophils and on human HL60 cells. The binding is Ca(2+)-dependent and requires the presence of sialic acid on the ligand. This P-selectin-ligand is not recognized by E-selectin. Removal of N-linked carbohydrate side chains from the 150-kD and the 160-kD monospecific selectin ligands abolishes the binding of both ligands to the respective selectin. Treatment of HL60 cells with Peptide: N-glycosidase F inhibited cell binding to P- and E-selectin. In addition, glycoproteins of 230 and 130 kD were found on mature mouse neutrophils, which bound both to E- and P-selectin in a Ca(2+)-dependent fashion. The signals detected for these ligands were 15-20-fold weaker than those for the monospecific ligands. Both proteins were heavily sialylated and selectin-binding was blocked by removal of sialic acid, but not by removal of N-linked carbohydrates. Our data reveal that E- and P-selectin recognize two categories of glycoprotein ligands: one type requires N-linked carbohydrates for binding and is monospecific for each of the two selectins and the other type binds independent of N-linked carbohydrates and is common for both endothelial selectins.
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15 April 1994
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April 15 1994
Monospecific and common glycoprotein ligands for E- and P-selectin on myeloid cells.
M Lenter,
M Lenter
Hans Spemann Laboratory, Max Planck Institute for Immunology, Freiburg, Germany.
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A Levinovitz,
A Levinovitz
Hans Spemann Laboratory, Max Planck Institute for Immunology, Freiburg, Germany.
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S Isenmann,
S Isenmann
Hans Spemann Laboratory, Max Planck Institute for Immunology, Freiburg, Germany.
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D Vestweber
D Vestweber
Hans Spemann Laboratory, Max Planck Institute for Immunology, Freiburg, Germany.
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M Lenter
Hans Spemann Laboratory, Max Planck Institute for Immunology, Freiburg, Germany.
A Levinovitz
Hans Spemann Laboratory, Max Planck Institute for Immunology, Freiburg, Germany.
S Isenmann
Hans Spemann Laboratory, Max Planck Institute for Immunology, Freiburg, Germany.
D Vestweber
Hans Spemann Laboratory, Max Planck Institute for Immunology, Freiburg, Germany.
Online ISSN: 1540-8140
Print ISSN: 0021-9525
J Cell Biol (1994) 125 (2): 471–481.
Citation
M Lenter, A Levinovitz, S Isenmann, D Vestweber; Monospecific and common glycoprotein ligands for E- and P-selectin on myeloid cells.. J Cell Biol 15 April 1994; 125 (2): 471–481. doi: https://doi.org/10.1083/jcb.125.2.471
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