Effects of the Flavoprotein Inhibitor, Diphenyleneiodonium Sulfate, on Ex Vivo Organic Nitrate Tolerance in the Rat

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Vol. 293, Issue 2, 569-577, May 2000

Effects of the Flavoprotein Inhibitor, Diphenyleneiodonium Sulfate, on Ex Vivo Organic Nitrate Tolerance in the Rat¹

Jodan D. Ratz, John J. McGuire, Diane J. Anderson and Brian M. Bennett

Department of Pharmacology and Toxicology, Faculty of Health Sciences, Queen's University, Kingston, Ontario, Canada

The flavoprotein inhibitor, diphenyleneiodonium (DPI), inhibits the action of glyceryl trinitrate (GTN) and the D-enantiomerof isoidide dinitrate (IIDN), but not the L-enantiomer (L-IIDN),in isolated rat aorta via inhibition of the bioactivation of theseprodrugs. Paradoxically, a vascular NAD(P)H oxidase, which alsois inhibited by DPI, has been proposed to generate superoxidethat quenches nitric oxide (NO) produced during GTN biotransformation,and increased oxidase levels are proposed to contribute to thephenomenon of organic nitrate tolerance. We examined the effectof DPI on isolated rat aorta using an in vivo model of organicnitrate tolerance. The EC₅₀ values for GTN-, D-IIDN-, and L-IIDN-inducedrelaxation of aorta from GTN-tolerant rats were increased 4.5-to 7.5-fold. Treatment of blood vessels with DPI (0.3 µM) increasedthe EC₅₀ values for GTN and D-IIDN by the same magnitude in controland tolerant aortae, a result that would not be predicted if DPIand GTN tolerance affected common targets. The expression of NADPH-cytochromeP450 reductase (CPR) during in vivo tolerance was assessed byNADPH-dependent cytochrome c reductase activity of aortic microsomes,immunoblotting, and Northern analysis. By all three determinants,CPR expression was unchanged in aorta from GTN-tolerant rats.Superoxide dismutase-inhibitable NADPH-dependent cytochrome creductase activity (a measure of superoxide generation) of tolerantrat aortic microsomes was not different from that of controls.Superoxide dismutase-inhibitable NADH-dependent cytochrome c reductaseactivity was detected only in microsomes from tolerant animals.DPI caused a modest increase in the sensitivity for relaxationby the NO donor DEA NONOate to an equal extent in tolerant andnontolerant tissues, whereas the superoxide scavenger, 4,5-dihydroxy-1,3-benzenedisulfonic acid (Tiron), had no effect on the sensitivity forrelaxation by GTN. These results would not be expected if tolerance-inducedincreases in superoxide were a causative factor for the reducedrelaxation response in tolerance. We conclude that neither reducedflavoprotein-dependent metabolic activation of organic nitrates,such as that mediated by CPR, nor increased superoxide due toincreased NAD(P)H oxidase activity can account for the developmentof in vivo tolerance to GTN.

¹ This work was supported by a grant (T2510) from the Heart and Stroke Foundation of Ontario. J.D.R. is a recipient of an OntarioGraduate Student scholarship and a Queen's Graduate Award. J.J.M.is a recipient of a Research Traineeship from the Heart and StrokeFoundation of Canada (HSFC). B.M.B. is a recipient of a CareerInvestigator award from theHSFC.

0022-3565/00/2932-0569$03.00/0
THE JOURNAL OF PHARMACOLOGY AND EXPERIMENTAL THERAPEUTICS
Copyright © 2000 by The American Society for Pharmacology and Experimental Therapeutics

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Effects of the Flavoprotein Inhibitor, Diphenyleneiodonium Sulfate, on Ex Vivo Organic Nitrate Tolerance in the Rat1

Effects of the Flavoprotein Inhibitor, Diphenyleneiodonium Sulfate, on Ex Vivo Organic Nitrate Tolerance in the Rat¹