This study examines the role of L-selectin in monocyte adhesion to arterial endothelium, a key pathogenic event of atherosclerosis. Using a nonstatic (rotation) adhesion assay, we observed that monocyte binding to bovine aortic endothelium at 4°C increased four to nine times upon endothelium activation with tumor necrosis factor (TNF)-α. mAb-blocking experiments demonstrated that L-selectin mediates a major part (64 ± 18%) of monocyte attachment. Videomicroscopy experiments performed under flow indicated that monocytes abruptly halted on 8-h TNF-α–activated aortic endothelium, ∼80% of monocyte attachment being mediated by L-selectin. Flow cytometric studies with a L-selectin/IgM heavy chain chimeric protein showed calcium-dependent L-selectin binding to cytokine-activated and, unexpectedly, unactivated aortic cells. Soluble L-selectin binding was completely inhibited by anti–L-selectin mAb or by aortic cell exposure to trypsin. Experiments with cycloheximide, chlorate, or neuraminidase showed that protein synthesis and sulfate groups, but not sialic acid residues, were essential for L-selectin counterreceptor function. Moreover, heparin lyases partially inhibited soluble L-selectin binding to cytokine-activated aortic cells, whereas a stronger inhibition was seen with unstimulated endothelial cells, suggesting that cytokine activation could induce the expression of additional ligand(s) for L-selectin, distinct from heparan sulfate proteoglycans. Under flow, endothelial cell treatment with heparinase inhibited by ∼80% monocyte attachment to TNF-α–activated aortic endothelium, indicating a major role for heparan sulfate proteoglycans in monocyte–endothelial interactions. Thus, L-selectin mediates monocyte attachment to activated aortic endothelium, and heparan sulfate proteoglycans serve as arterial ligands for monocyte L-selectin.
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24 February 1997
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February 24 1997
Monocyte Adhesion to Activated Aortic Endothelium: Role of L-Selectin and Heparan Sulfate Proteoglycans
Laura Giuffrè,
Laura Giuffrè
*Division of Hematology, the Hematology Central Laboratory of the University of Lausanne, 1011-CHUV Lausanne; and ‡Biomedical Engineering Laboratory of the Swiss Federal Institute of Technology, 1015-PSE-Ecublens, Switzerland
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Anne-Sophie Cordey,
Anne-Sophie Cordey
*Division of Hematology, the Hematology Central Laboratory of the University of Lausanne, 1011-CHUV Lausanne; and ‡Biomedical Engineering Laboratory of the Swiss Federal Institute of Technology, 1015-PSE-Ecublens, Switzerland
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Natacha Monai,
Natacha Monai
*Division of Hematology, the Hematology Central Laboratory of the University of Lausanne, 1011-CHUV Lausanne; and ‡Biomedical Engineering Laboratory of the Swiss Federal Institute of Technology, 1015-PSE-Ecublens, Switzerland
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Yanik Tardy,
Yanik Tardy
*Division of Hematology, the Hematology Central Laboratory of the University of Lausanne, 1011-CHUV Lausanne; and ‡Biomedical Engineering Laboratory of the Swiss Federal Institute of Technology, 1015-PSE-Ecublens, Switzerland
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Marc Schapira,
Marc Schapira
*Division of Hematology, the Hematology Central Laboratory of the University of Lausanne, 1011-CHUV Lausanne; and ‡Biomedical Engineering Laboratory of the Swiss Federal Institute of Technology, 1015-PSE-Ecublens, Switzerland
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Olivier Spertini
Olivier Spertini
*Division of Hematology, the Hematology Central Laboratory of the University of Lausanne, 1011-CHUV Lausanne; and ‡Biomedical Engineering Laboratory of the Swiss Federal Institute of Technology, 1015-PSE-Ecublens, Switzerland
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Laura Giuffrè
,
Anne-Sophie Cordey
,
Natacha Monai
,
Yanik Tardy
,
Marc Schapira
,
Olivier Spertini
*Division of Hematology, the Hematology Central Laboratory of the University of Lausanne, 1011-CHUV Lausanne; and ‡Biomedical Engineering Laboratory of the Swiss Federal Institute of Technology, 1015-PSE-Ecublens, Switzerland
Please address all correspondence to Dr. Olivier Spertini, Division of Hematology, University of Lausanne, 1011-CHUV Lausanne, Switzerland.
Received:
June 04 1996
Revision Received:
October 15 1996
Online ISSN: 1540-8140
Print ISSN: 0021-9525
1997
J Cell Biol (1997) 136 (4): 945–956.
Article history
Received:
June 04 1996
Revision Received:
October 15 1996
Citation
Laura Giuffrè, Anne-Sophie Cordey, Natacha Monai, Yanik Tardy, Marc Schapira, Olivier Spertini; Monocyte Adhesion to Activated Aortic Endothelium: Role of L-Selectin and Heparan Sulfate Proteoglycans. J Cell Biol 24 February 1997; 136 (4): 945–956. doi: https://doi.org/10.1083/jcb.136.4.945
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