Author:
Kevil Christopher G.,Chidlow John H.,Bullard Daniel C.,Kucik Dennis F.
Abstract
Leukocyte rolling, adhesion, and migration on vascular endothelium involve several sets of adhesion molecules that interact simultaneously. Each of these receptor-ligand pairs may play multiple roles. We examined the role of ICAM-1 in adhesive interactions with mouse aortic endothelial cells (MAECs) in an in vitro flow system. Average rolling velocity of the monocytic cell line WEHI 274.1 was increased on ICAM-1-deficient MAECs compared with wild-type MAECs, both with and without TNF-α stimulation. High-temporal-resolution analysis provided insights into the underlying basis for these differences. Without TNF-α stimulation, average rolling velocity was slower on wild-type than on ICAM-1-deficient endothelium because of brief (<1 s) pauses. On TNF-α-stimulated ICAM-1-deficient endothelium, cells rolled faster because of transient accelerations, producing “jerky” rolling. Firm adhesion to ICAM-1-deficient MAECs was significantly reduced compared with wild-type MAECs, although the number of rolling cells was similar. These results demonstrate directly that ICAM-1 affects rolling velocity by stabilizing leukocyte rolling.
Publisher
American Physiological Society
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