Role of calcium and calmodulin in flow-induced nitric oxide production in endothelial cells

MJ Kuchan, JA Frangos - American Journal of Physiology …, 1994 - journals.physiology.org
MJ Kuchan, JA Frangos
American Journal of Physiology-Cell Physiology, 1994journals.physiology.org
These experiments demonstrate that exposure of cultured endothelial cells (EC) to well-
defined laminar fluid flow results in an elevated rate of NO production. NO production was
monitored by release of NOx (NO2-+ NO3 (2-) and by cellular guanosine 3', 5'-cyclic
monophosphate (cGMP) concentration. NO synthase (NOS) inhibitor blocked the flow-
mediated stimulation of both NOx and cGMP, indicating that both measurements reflect NO
production. Exposure to laminar flow increased NO release in a biphasic manner, with an …
These experiments demonstrate that exposure of cultured endothelial cells (EC) to well-defined laminar fluid flow results in an elevated rate of NO production. NO production was monitored by release of NOx (NO2- + NO3(2-) and by cellular guanosine 3',5'-cyclic monophosphate (cGMP) concentration. NO synthase (NOS) inhibitor blocked the flow-mediated stimulation of both NOx and cGMP, indicating that both measurements reflect NO production. Exposure to laminar flow increased NO release in a biphasic manner, with an initial rapid production consequent to the onset of flow followed by a less rapid, sustained production. A similar rapid increase in NO production resulted from an increase in flow above a preexisting level. The rapid initial production of NO was not dependent on shear stress within a physiological range (6-25 dyn/cm2) but may be dependent on the rate of change in shear stress. The sustained release of NO was dependent on physiological levels of shear stress. The calcium (Ca2+) or calmodulin (CaM) dependence of the initial and sustained production of NO was compared with bradykinin (BK)-mediated NO production. Both BK and the initial production were inhibited by Ca2+ and CaM antagonists. In contrast, the sustained shear stress-mediated NO production was not affected, despite the continued functional presence of the antagonists. Dexamethasone had no effect on either the initial or the sustained shear stress-mediated NO production. An inducible NOS does not, therefore, explain the apparent Ca2+/CaM independence of the sustained shear stress-mediated NO production.(ABSTRACT TRUNCATED AT 250 WORDS)
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