Selective nitros(yl)ation induced in vivo by a nitric oxide-donating cyclooxygenase-2 inhibitor: A NObonomic analysis

被引:16
作者
Dhawan, V [1 ]
Schwalb, DJ [1 ]
Shumway, MJ [1 ]
Warren, MC [1 ]
Wexler, RS [1 ]
Zemtseva, IS [1 ]
Zifcak, BM [1 ]
Janero, DR [1 ]
机构
[1] NitrMed Inc, Lexington, MA 02421 USA
关键词
anti-inflammatory medicine; carbonates; carbonic anhydrase; cyclooxygenase; drugs; erythrocyte; metabolic profiling; metabonomics; nitrate; nitric oxide; nitric oxide donor; nitrite; nitrosation; nitrosylation; NO-coxib; organic nitrate; free radicals;
D O I
10.1016/j.freeradbiomed.2005.06.011
中图分类号
Q5 [生物化学]; Q7 [分子生物学];
学科分类号
071010 ; 081704 ;
摘要
Nitric oxide (NO) enhances anti-inflammatory drug action. Through a metabonomics approach termed "NObonomics," the effects of a prototypic NO donor (organic nitrate)-cyclooxygenase-2 inhibitor hybrid (NO-coxib), NMI-1093, on the NO metabolite status of the circulation and major organs have been profiled in vivo in the rat. An oral anti-inflammatory NMI-1093 bolus elicited acute tissue-, time-, and dose-dependent changes in oxidative and nitroso/nitrosyl NO metabolites. Gastric N-nitrosation and hepatic S-nitrosation and heme nitrosylation emerged as sensitive indices of this NO-coxib's metabolism. Acute NMI-1093-induced nitros(yl)ation correlated positively as a function of nitrate plus nitrite formation across all organs examined, suggesting a Unifying in vivo mechanism consequent to NMI-1093 biotransformation that links oxidative and nitros(yl)ative routes of NO chemical biology and thereby may support downstream NO signaling. NMI-1093 depressed erythrocyte nitros(yl)ation, likely by inhibiting cellular carbonic anhydrase and shifting the intracellular balance between nitrogen oxides and carbonates. Glutathione-S-transferase or cytochrome P450 inhibitors also attenuated NMI-1093's NO metabolism in a compartment-selective fashion. Although not itself a NO donor, the des-nitro coxib analog of NMI-1093 influenced basal NO metabolite profiles, implicating a cyclooxygenase-NO synthase interaction in physiological NO regulation. By detailing the global NO metrics of a unique coxib bearing a popular NO-donor pharmacophore (i.e., a nitrate moiety) and defining some critical mechanistic determinants, this study demonstrates how NObonomics can serve as valuable tool in helping elucidate NO systems biology and the effect of NO-donor and non-NO-donating therapeutics thereon. (c) 2005 Elsevier Inc. All rights reserved.
引用
收藏
页码:1191 / 1207
页数:17
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