EVALUATION OF THE ABILITY OF THE ANGIOTENSIN-CONVERTING ENZYME-INHIBITOR CAPTOPRIL TO SCAVENGE REACTIVE OXYGEN SPECIES

被引：66

作者：

ARUOMA, OI ^{[1
]}

AKANMU, D ^{[1
]}

CECCHINI, R ^{[1
]}

HALLIWELL, B ^{[1
]}

机构：

[1] UNIV CALIF DAVIS,SACRAMENTO MED CTR,MED CTR,DIV PULM CRIT CARE MED,SACRAMENTO,CA 95817

来源：

CHEMICO-BIOLOGICAL INTERACTIONS | 1991年 / 77卷 / 03期

关键词：

CAPTOPRIL; ANTIOXIDANT; REPERFUSION INJURY; HYDROXYL RADICAL; SUPEROXIDE; HYPOCHLOROUS ACID;

D O I：

10.1016/0009-2797(91)90039-A

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：

Captopril, an inhibitor of angiotensin-converting enzyme, has been suggested to have additional cardioprotective action because of its ability to act as an antioxidant. The rates of reaction of captopril with several biologically-relevant reactive oxygen species were determined. Captopril reacts slowly, if at all, with superoxide (rate constant < 10(3) M-1 s-1) or hydrogen peroxide (rate constant < 1 M-1 s-1). It does not inhibit peroxidation of lipids stimulated by iron ions and ascorbate or by the myoglobin/H2O2 system. Indeed, mixtures of ferric ion and captopril can stimulate lipid peroxidation. Captopril reacts rapidly with hydroxyl radical (rate constant > 10(9) M-1 s-1) but might be unlikely to compete with most biological molecules for .OH because of the low concentration of captopril that can be achieved in vivo during therapeutic use. Captopril did not significantly inhibit iron ion-dependent generation of hydroxyl radicals from hydrogen peroxide. By contrast, captopril is a powerful scavenger of hypochlorous acid: it was able to protect alpha-1-antiproteinase (alpha-1AP) against inactivation by this species and to prevent formation of chloramines from taurine. We suggest that the antioxidant action of captopril in vivo is likely to be limited, and may be restricted to protection against damage by hypochlorous acid derived from the action of neutrophil myeloperoxidase.

引用

页码：303 / 314

页数：12

共 42 条

[1] BINDING OF IRON(II) IONS TO THE PENTOSE SUGAR 2-DEOXYRIBOSE [J].

ARUOMA, OI ;

CHAUDHARY, SS ;

GROOTVELD, M ;

HALLIWELL, B .

JOURNAL OF INORGANIC BIOCHEMISTRY, 1989, 35 (02) :149-155

[2] THE ROLE OF IRON IN ASCORBATE-DEPENDENT DEOXYRIBOSE DEGRADATION - EVIDENCE CONSISTENT WITH A SITE-SPECIFIC HYDROXYL RADICAL GENERATION CAUSED BY IRON IONS BOUND TO THE DEOXYRIBOSE MOLECULE [J].

ARUOMA, OI ;

GROOTVELD, M ;

HALLIWELL, B .

JOURNAL OF INORGANIC BIOCHEMISTRY, 1987, 29 (04) :289-299

[3] THE ANTIOXIDANT ACTION OF N-ACETYLCYSTEINE - ITS REACTION WITH HYDROGEN-PEROXIDE, HYDROXYL RADICAL, SUPEROXIDE, AND HYPOCHLOROUS ACID [J].

ARUOMA, OI ;

HALLIWELL, B ;

HOEY, BM ;

BUTLER, J .

FREE RADICAL BIOLOGY AND MEDICINE, 1989, 6 (06) :593-597

[4] APPARENT INACTIVATION OF ALPHA-1-ANTIPROTEINASE BY SULFUR-CONTAINING RADICALS DERIVED FROM PENICILLAMINE [J].

ARUOMA, OI ;

HALLIWELL, B ;

BUTLER, J ;

HOEY, BM .

BIOCHEMICAL PHARMACOLOGY, 1989, 38 (24) :4353-4357

[5] ENHANCED PROSTAGLANDIN PRODUCTION IN THE ISCHEMIC-REPERFUSED MYOCARDIUM BY CAPTOPRIL LINKED WITH ITS FREE-RADICAL SCAVENGING ACTION [J].

BAGCHI, D ;

IYENGAR, J ;

STOCKWELL, P ;

DAS, DK .

PROSTAGLANDINS LEUKOTRIENES AND ESSENTIAL FATTY ACIDS, 1989, 38 (02) :145-150

[6] DIRECT SCAVENGING OF FREE-RADICALS BY CAPTOPRIL, AN ANGIOTENSIN CONVERTING ENZYME-INHIBITOR [J].

BAGCHI, D ;

PRASAD, R ;

DAS, DK .

BIOCHEMICAL AND BIOPHYSICAL RESEARCH COMMUNICATIONS, 1989, 158 (01) :52-57

[7] SUPEROXIDE DISMUTASE - IMPROVED ASSAYS AND AN ASSAY APPLICABLE TO ACRYLAMIDE GELS [J].

BEAUCHAM.C ;

FRIDOVIC.I .

ANALYTICAL BIOCHEMISTRY, 1971, 44 (01) :276-&

[8] REACTIVITY OF HO2/O-2 RADICALS IN AQUEOUS-SOLUTION [J].

BIELSKI, BHJ ;

CABELLI, DE ;

ARUDI, RL ;

ROSS, AB .

JOURNAL OF PHYSICAL AND CHEMICAL REFERENCE DATA, 1985, 14 (04) :1041-1100

[9] OXYGEN-DERIVED FREE-RADICALS AND POSTISCHEMIC MYOCARDIAL DYSFUNCTION (STUNNED MYOCARDIUM) [J].

BOLLI, R .

JOURNAL OF THE AMERICAN COLLEGE OF CARDIOLOGY, 1988, 12 (01) :239-249

[10] MARKED REDUCTION OF FREE-RADICAL GENERATION AND CONTRACTILE DYSFUNCTION BY ANTIOXIDANT THERAPY BEGUN AT THE TIME OF REPERFUSION - EVIDENCE THAT MYOCARDIAL STUNNING IS A MANIFESTATION OF REPERFUSION INJURY [J].

BOLLI, R ;

JEROUDI, MO ;

PATEL, BS ;

ARUOMA, OI ;

HALLIWELL, B ;

LAI, EK ;

MCCAY, PB .

CIRCULATION RESEARCH, 1989, 65 (03) :607-622

← 1 2 3 4 5 →