CHROMIUM(VI) REDUCTION BY ASCORBATE - ROLE OF REACTIVE INTERMEDIATES IN DNA-DAMAGE IN-VITRO

被引：51

作者：

STEARNS, DM ^{[1
]}

COURTNEY, KD ^{[1
]}

GIANGRANDE, PH ^{[1
]}

PHIEFFER, LS ^{[1
]}

WETTERHAHN, KE ^{[1
]}

机构：

[1] DARTMOUTH COLL,DEPT CHEM,6128 BURKE LAB,HANOVER,NH 03755

来源：

ENVIRONMENTAL HEALTH PERSPECTIVES | 1994年 / 102卷

关键词：

CHROMIUM(VI); CHROMIUM(V); ASCORBATE; SPIN TRAPPING; FREE RADICALS; DNA DAMAGE;

D O I：

10.2307/3431756

中图分类号：

X [环境科学、安全科学];

学科分类号：

08 ; 0830 ;

摘要：

Reaction of chromium(VI) with one equivalent of ascorbate was studied by electron paramagnetic resonance spectroscopy in the presence of 0.10 M 5,5-dimethyl-1-pyrroline-1-oxide (DMPO) at room temperature in 0.10 M [N-[2-hydroxyethyl]piperazine-N'-[2-ethanesulfonic acid)] (HEPES) and 0.05 M tris(hydroxymethyl)aminomethane hydrochloride (Tris-HCl) buffers (pH 7.0, room temperature). Chromium(V), ascorbyl radical, and carbon-based DMPO-radical adducts were observed. A higher level of Cr(V) was observed in HEPES buffer and a higher level of the DMPO-radical adducts was observed in Tris-HCl buffer. Chromium-DNA binding studies were carried out in vitro for calf thymus DNA incubated with Cr(VI) and ascorbate in both buffets at 37 degrees C. Higher Cr-DNA binding was observed in HEPES buffer. DNA strand-break studies were carried out in vitro on pBR322 DNA incubated with Cr(VI) and ascorbate in both buffers at 37 degrees C. Higher percent nicking was observed in Tris-HCl buffer. Addition of DMPO decreased nicking levels in Tris-HCl buffer. These results suggest that free radicals are more reactive than Cr(V) in producing DNA strand breaks and that Cr(V) will react with DNA to produce Cr-DNA adducts. The fact that buffer affects the nature of the reactive intermediates produced upon reduction of Cr(V) may be related to differences in intracellular metabolism of Cr(VI) and resulting DNA damage observed in various cell culture systems and animal tissues in vivo.

引用

页码：21 / 25

页数：5

共 22 条

[1]

AIYAR J, 1991, ENVIRON HEALTH PERSP, V92, P53, DOI 10.1289/ehp.919253

[2]

Alcedo J A, 1990, Int Rev Exp Pathol, V31, P85

[3] ACTIVATION OF CHROMIUM(VI) BY THIOLS RESULTS IN CHROMIUM(V) FORMATION, CHROMIUM BINDING TO DNA AND ALTERED DNA CONFORMATION [J].

BORGES, KM ;

BOSWELL, JS ;

LIEBROSS, RH ;

WETTERHAHN, KE .

CARCINOGENESIS, 1991, 12 (04) :551-561

[4]

CONNETT PH, 1983, STRUCT BOND, V54, P93

[5] PARAMAGNETIC-RESONANCE, MAGNETIC-SUSCEPTIBILITY, AND ANTI-FERROMAGNETIC EXCHANGE IN A CR-5+ PARAMAGNET - POTASSIUM PERCHROMATE (K3CRO8) [J].

DALAL, NS ;

MILLAR, JM ;

JAGADEESH, MS ;

SEEHRA, MS .

JOURNAL OF CHEMICAL PHYSICS, 1981, 74 (03) :1916-1923

[6]

De Flora S, 1989, LIFE CHEM REPORTS, V7, P169

[7] CHROMIUM(V)-INDUCED CLEAVAGE OF DNA - ARE CHROMIUM(V) COMPLEXES THE ACTIVE CARCINOGENS IN CHROMIUM(VI)-INDUCED CANCERS [J].

FARRELL, RP ;

JUDD, RJ ;

LAY, PA ;

DIXON, NE ;

BAKER, RSU ;

BONIN, AM .

CHEMICAL RESEARCH IN TOXICOLOGY, 1989, 2 (04) :227-229

[8] ELECTRON-PARAMAGNETIC-RES STUDY OF THE CR(V) AND RADICAL SPECIES PRODUCED IN THE REDUCTION OF CR(VI) BY ASCORBATE [J].

GOODGAME, DML ;

JOY, AM .

INORGANICA CHIMICA ACTA-BIOINORGANIC CHEMISTRY, 1987, 135 (02) :115-118

[9] CHROMIUM (VI)-INDUCED DNA DAMAGE IN CHICK-EMBRYO LIVER AND BLOOD-CELLS INVIVO [J].

HAMILTON, JW ;

WETTERHAHN, KE .

CARCINOGENESIS, 1986, 7 (12) :2085-2088

[10] ELECTRON-SPIN RESONANCE STUDY OF SPIN ADDUCTS OF OH AND HO2 RADICALS WITH NITRONES IN ULTRAVIOLET PHOTOLYSIS OF AQUEOUS HYDROGEN-PEROXIDE SOLUTIONS [J].

HARBOUR, JR ;

CHOW, V ;

BOLTON, JR .

CANADIAN JOURNAL OF CHEMISTRY-REVUE CANADIENNE DE CHIMIE, 1974, 52 (20) :3549-3553

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