INDUCTION OF LUNG-SPECIFIC DNA-DAMAGE BY METABOLICALLY METHYLATED ARSENICS VIA THE PRODUCTION OF FREE-RADICALS

被引：108

作者：

YAMANAKA, K ^{[1
]}

OKADA, S ^{[1
]}

机构：

[1] UNIV SHIZUOKA,SCH PHARMACEUT SCI,DEPT RADIOBIOCHEM,SHIZUOKA 422,JAPAN

来源：

ENVIRONMENTAL HEALTH PERSPECTIVES | 1994年 / 102卷

关键词：

DNA DAMAGE; SINGLE-STRAND BREAKS; METHYLATED ARSENICS; FREE RADICALS; DIMETHYLARSENIC PEROXYL RADICAL; DIMETHYLARSINE;

D O I：

10.2307/3431760

中图分类号：

X [环境科学、安全科学];

学科分类号：

08 ; 0830 ;

摘要：

To clarify the genotoxicity of inorganic arsenics, we focused on the genotoxic effect of metabolically methylated arsenics in mammals. Oral administration to mice of dimethylarsinic acid (DMAA), a major metabolite of inorganic arsenics, induced lung-specific DNA damage, i.e., DNA single-strand breaks and the clumping of heterochromatin. The lung-specific strand breaks were not caused by DMAA itself, but by dimethylarsine, a further metabolite of DMAA. An in vitro experiment indicated that DNA single-strand breaks by dimethylarsine were suppressed by the presence of superoxide dismutase and catalase, suggesting that the strand breaks were induced via the production of free-radical species including active oxygens. Dimethylarsenic peroxyl radical [(CH3)(2)AsOO.] and superoxide anion radical produced from the reaction between molecular oxygen acid dimethylarsine were detected by electron-spin resonance analysis using a spin-trapping agent and the cytochrome-c method, respectively. Of these two radicals, the dimethylarsenic peroxyl radical rather than the superoxide anion radical is assumed to play the dominant role in causing the DNA damage, at least for DNA single-strand breaks.

引用

页码：37 / 40

页数：4

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