Rat aortic ring preparations were mounted in organ baths, exposed to cobalt chloride (0.3–300 μmol/L) for 30 min, and then subjected to contractile agents or relaxants 1 and 5 h after the end of exposure. Presence of cobalt chloride did not affect the contractile response to phenylephrine. Brief exposure to cobalt chloride, however, even at 5 h after the end of exposure, not only augmented contractile responses to KCl or phenylephrine but also attenuated the relaxant response to acetylcholine. The mechanical denudation of endothelium or inhibition of endothelial nitric oxide synthase with 100 μmol/L Nω-nitro-l-arginine methyl ester abolished the augmentation of contractile responses. Pre-treatment with 150 units/mL of superoxide dismutase also abrogated the augmented contractile responses. Brief exposure to cobalt chloride did not affect the contractile response to phorbol dibutyrate in the presence or absence of calcium, or the expression of HSP70.
In conclusion, endothelial dysfunction plays an important role in the augmentation of aortic contractility, after brief exposure to cobalt chloride.