Differential effects of phosphodiesterase PDE-3/PDE-4-specific inhibitors on vasoconstriction and cAMP-dependent vasorelaxation following balloon angioplasty

doi:10.1152/ajpheart.00419.2006

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Am J Physiol Heart Circ Physiol 292: H2973-H2981, 2007. First published February 9, 2007; doi:10.1152/ajpheart.00419.2006
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Differential effects of phosphodiesterase PDE-3/PDE-4-specific inhibitors on vasoconstriction and cAMP-dependent vasorelaxation following balloon angioplasty

Hong Zhao, John Quilley, David C. Montrose, Swarna Rajagopalan, Qizhi Guan, and Carolyn J. Smith

Department of Pharmacology, New York Medical College, Valhalla, New York

Submitted 26 April 2006 ; accepted in final form 9 February 2007

It is known that cAMP and cGMP are important for vasorelaxation,and cyclic nucleotide phosphodiesterases (PDEs) regulate theirlevels. Balloon angioplasty (BAL) is associated with reducedcAMP and cGMP levels, and inhibition of PDE-3 reduces restenosis.In this study, we found that BAL increased PDE-3 activity, whichaffected vasoreactivity of rat aortic rings 24-h post-BAL; thesewere compared with intact (INT) and ex vivo endothelium-denudedrings (RUB) from sham rats. In BAL and RUB rings, vasorelaxantresponses to ACh were abolished. The EC₅₀ for phenylephrine(PE) was 1.8-fold less in RUB than in INT or BAL, whereas themaximal contractile effect of PE was greater in BAL than inINT or RUB. PDE-3 inhibitors reduced the maximal response toPE by >65% in BAL compared with 10–30% in INT and RUB;the reduction of the maximal response to U-46619 was 37% inBAL compared with 8% in INT with no reduction in RUB. PDE-4inhibitors reduced PE-induced tone by <30% in an endothelium-dependentmanner. Vasorelaxant responses to agonists that utilize cAMPwere greatly impaired in BAL and RUB rings, and inhibition ofPDE-3 enhanced the vasorelaxant responses in BAL or RUB. Inhibitionof PDE-4 increased vasorelaxant responses to isoproterenol (ISO)to a much lesser degree. Thus PDE-3 and PDE-4 inhibitors exhibiteddifferential effects on PE-induced tone and vasorelaxant responsesto ISO. Inhibition of PDE-3 also produced a greater increasein cAMP in BAL than INT or RUB rings. These results suggestthat increased PDE-3 activity after BAL may promote a vasospasticstate and that the reduction in cAMP may, possibly, influencevessel remodeling.

rat aorta; cyclic adenosine 3', 5'-cyclic monophosphate

Address for reprint requests and other correspondence: H. Zhao, Dept. of Pharmacology, New York Medical College, Valhalla, NY 10595 (e-mail: hong_zhao{at}nymc.edu)