INHIBITION OF MACROPHAGE AND ENDOTHELIAL-CELL NITRIC-OXIDE SYNTHASE BY DIPHENYLENEIODONIUM AND ITS ANALOGS

被引：451

作者：

STUEHR, DJ ^{[1
]}

FASEHUN, OA ^{[1
]}

KWON, NS ^{[1
]}

GROSS, SS ^{[1
]}

GONZALEZ, JA ^{[1
]}

LEVI, R ^{[1
]}

NATHAN, CF ^{[1
]}

机构：

[1] CORNELL UNIV,MED CTR,COLL MED,DEPT PHARMACOL,NEW YORK,NY 10021

来源：

FASEB JOURNAL | 1991年 / 5卷 / 01期

关键词：

L-ARGININE; FAD; FLAVOPROTEIN; INTERFERON-GAMMA; ENDOTHELIUM-DERIVED RELAXING FACTOR;

D O I：

10.1096/fasebj.5.1.1703974

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：

The cofactor requirements of macrophage nitric oxide (NO.) synthase suggest involvement of an NADPH-dependent flavoprotein. This prompted us to test the effect of the flavoprotein inhibitors diphenyleneiodonium (DPI), di-2-thienyliodonium (DTI), and iodoniumdiphenyl (ID) on the NO. synthases of macrophages and endothelium. DPI, DTI, and ID completely inhibited NO. synthesis by mouse macrophages, their lysates, and partially purified macrophage NO. synthase. Inhibiton of NO. synthase by these agents was potent (IC50's 50-150 nM), irreversible, dependent on time and temperature, and independent of enzyme catalysis. The inhibition by DPI was blocked by NADPH, NADP+, or 2'5'-ADP, but not by NADH. Likewise, FAD or FMN, but not riboflavin or adenosine 5-diphosphoribose, protected NO. synthase from inhibition by DPI. Neither NADPH nor FAD reacted with DPI. Once NO. synthase was inhibited by DPI, neither NADPH nor FAD could restore its activity. DPI also inhibited acetylcholine-induced relaxation of norepinephrine-preconstricted rabbit aortic rings (IC50 300 nM). Inhibition of acetylcholine-induced relaxation persisted for at least 2 h after DPI was washed out. In contrast, DPI had no effect on norepinephrine-induced vasoconstriction itself nor on vasorelaxation induced by the NO.-generating agent sodium nitroprusside. These results suggest that NO. synthesis in both macrophages and endothelial cells depends on an NADPH-utilizing flavoprotein. As a new class of NO. synthase inhibitors, DPI and its analogs are likely to prove useful in analyzing the physiologic and pathophysiologic roles of NO..

引用

页码：98 / 103

页数：6

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