A mechanism of paraquat toxicity involving nitric oxide synthase

被引:147
作者
Day, BJ [1 ]
Patel, M
Calavetta, L
Chang, LY
Stamler, JS
机构
[1] Natl Jewish Med & Res Ctr, Dept Med, Denver, CO 80206 USA
[2] Univ Colorado, Hlth Sci Ctr, Dept Pharmaceut Sci, Sch Pharm, Denver, CO 80206 USA
[3] Duke Univ, Med Ctr, Howard Hughes Med Inst, Dept Cell Biol,Div Pulm, Durham, NC 27710 USA
[4] Duke Univ, Med Ctr, Howard Hughes Med Inst, Dept Med,Div Cardiol, Durham, NC 27710 USA
[5] Duke Univ, Med Ctr, Howard Hughes Med Inst, Dept Cell Biol,Div Cardiol, Durham, NC 27710 USA
[6] Duke Univ, Med Ctr, Howard Hughes Med Inst, Dept Med,Div Pulm, Durham, NC 27710 USA
来源
PROCEEDINGS OF THE NATIONAL ACADEMY OF SCIENCES OF THE UNITED STATES OF AMERICA | 1999年 / 96卷 / 22期
关键词
D O I
10.1073/pnas.96.22.12760
中图分类号
O [数理科学和化学]; P [天文学、地球科学]; Q [生物科学]; N [自然科学总论];
学科分类号
07 ; 0710 ; 09 ;
摘要
(PQ) is a well described pneumotoxicant that produces toxicity by redox cycling with cellular diaphorases, thereby elevating intracellular levers of superoxide O-2(radical anion). NO synthase (NOS) has been shown to participate in PQ-induced lung injury. Current theory holds that NO reacts with O-2(radical anion) generated by PQ to produce the toxin peroxynitrite. We asked whether NOS might alternatively function as a PO diaphorase and reexamined the question of whether NO/O-2(radical anion) reactions were toxic or protective. Here, we show that: (i) neuronal NOS has PQ diaphorase activity that inversely correlates with NO formation; (ii) PQ-induced endothelial cell toxicity is attenuated by inhibitors of NOS that prevent NADPH oxidation, but is not attenuated by those that do not; (iii) PQ inhibits endothelium-derived, but not NO-induced, relaxations of aortic rings; and (iv) PQ-induced cytotoxicity is potentiated in cytokine-activated macrophages in a manner that correlates with its ability to block NO formation. These data indicate that NOS is a PO diaphorase and that toxicity of such redox-active compounds involves a loss of NO-related activity.
引用
收藏
页码:12760 / 12765
页数:6
相关论文
共 44 条
[1]   NITRIC-OXIDE MEDIATES OXIDANT TISSUE-INJURY CAUSED BY PARAQUAT AND XANTHINE-OXIDASE [J].
BERISHA, H ;
PAKBAZ, H ;
ABSOOD, A ;
FODA, HD ;
SAID, SI .
CELLULAR, BIOCHEMICAL, AND MOLECULAR ASPECTS OF REPERFUSION INJURY, 1994, 723 :422-425
[2]   NITRIC-OXIDE AS A MEDIATOR OF OXIDANT LUNG INJURY DUE TO PARAQUAT [J].
BERISHA, HI ;
PAKBAZ, H ;
ABSOOD, A ;
SAID, SI .
PROCEEDINGS OF THE NATIONAL ACADEMY OF SCIENCES OF THE UNITED STATES OF AMERICA, 1994, 91 (16) :7445-7449
[3]   NITRIC-OXIDE, A NOVEL NEURONAL MESSENGER [J].
BREDT, DS ;
SNYDER, SH .
NEURON, 1992, 8 (01) :3-11
[4]   CLONED AND EXPRESSED NITRIC-OXIDE SYNTHASE STRUCTURALLY RESEMBLES CYTOCHROME-P-450 REDUCTASE [J].
BREDT, DS ;
HWANG, PM ;
GLATT, CE ;
LOWENSTEIN, C ;
REED, RR ;
SNYDER, SH .
NATURE, 1991, 351 (6329) :714-718
[5]  
BROOKS RE, 1971, LAB INVEST, V25, P536
[6]   SUPEROXIDE-CATALYZED AND SINGLET OXYGEN-CATALYZED LIPID PEROXIDATION AS A POSSIBLE MECHANISM FOR PARAQUAT (METHYL VIOLOGEN) TOXICITY [J].
BUS, JS ;
GIBSON, JE ;
AUST, SD .
BIOCHEMICAL AND BIOPHYSICAL RESEARCH COMMUNICATIONS, 1974, 58 (03) :749-755
[7]   SYNERGISTIC INTERACTIONS BETWEEN NADPH CYTOCHROME-P-450 REDUCTASE, PARAQUAT, AND IRON IN THE GENERATION OF ACTIVE OXYGEN RADICALS [J].
CLEJAN, L ;
CEDERBAUM, AI .
BIOCHEMICAL PHARMACOLOGY, 1989, 38 (11) :1779-1786
[8]   PROTECTION OF CHINESE-HAMSTER OVARY CELLS FROM PARAQUAT-MEDIATED CYTO-TOXICITY BY A LOW-MOLECULAR WEIGHT MIMIC OF SUPEROXIDE-DISMUTASE (DF-MN) [J].
DARR, DJ ;
YANNI, S ;
PINNELL, SR .
FREE RADICAL BIOLOGY AND MEDICINE, 1988, 4 (06) :357-363
[9]   NITRIC-OXIDE SYNTHASE AND NEURONAL NADPH DIAPHORASE ARE IDENTICAL IN BRAIN AND PERIPHERAL-TISSUES [J].
DAWSON, TM ;
BREDT, DS ;
FOTUHI, M ;
HWANG, PM ;
SNYDER, SH .
PROCEEDINGS OF THE NATIONAL ACADEMY OF SCIENCES OF THE UNITED STATES OF AMERICA, 1991, 88 (17) :7797-7801
[10]   A metalloporphyrin superoxide dismutase mimetic protects against paraquat-induced lung injury in vivo [J].
Day, BJ ;
Crapo, JD .
TOXICOLOGY AND APPLIED PHARMACOLOGY, 1996, 140 (01) :94-100
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