Department of Hematology, University Hospital Utrecht, The
Netherlands.
Abstract
BACKGROUND: Nitric oxide (NO)
has been identified as endothelium-derived relaxing factor (EDRF), which,
in addition to its relaxant effects on vascular smooth muscle cells, is
also a potent inhibitor of platelet aggregation. An inhibitory role on
platelet adhesion has been suggested from experiments with washed
platelets under static conditions. We have determined whether
endothelium-derived and exogenous NO also regulates platelet adhesion in
whole blood under flow conditions.
METHODS AND RESULTS: The effect
of endothelium-derived NO was studied by the addition of specific
inhibitors of NO production, L-N-monomethyl arginine (L-NMMA) and N-iminoethyl-L-ornithine
(L-NIO), to a perfusion system in which both endothelial cells and their
matrices were present. A concentration-dependent increase in platelet
adhesion to the matrix was found with a maximum inhibition at a
concentration of 2 mM L-NMMA and 0.1 mM L-NIO. The effect was dependent on
the presence of endothelial cells, because no increase in platelet
adhesion was observed in their absence. The effect of exogenous NO was
tested in a specially devised perfusion system in which the NO was
introduced at the site of adhesion by means of a porous membrane on which
an extracellular matrix of endothelial cells was present. Inhibition of
platelet adhesion by NO was found at all shear rates tested and after all
perfusion periods.
CONCLUSIONS: These results
demonstrate that NO is a potent inhibitor of platelet adhesion under flow
conditions and thereby contributes to the regulatory role of vascular
endothelial cells on platelet-vessel wall interaction.