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首页> 外文期刊>journal of applied toxicology >Effect of chemical form, route of administration and vehicle on 3,5‐dichloroaniline‐induced nephrotoxicity in the fischer 344 rat
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Effect of chemical form, route of administration and vehicle on 3,5‐dichloroaniline‐induced nephrotoxicity in the fischer 344 rat

机译:Effect of chemical form, route of administration and vehicle on 3,5‐dichloroaniline‐induced nephrotoxicity in the fischer 344 rat

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AbstractChloroanilines are widely used chemical intermediates for the manufacture of dyes, agricultural chemicals and industrial compounds. Nephrotoxicity occurs as one toxicity following intraperitoneal (i.p.) administration of chloroaniline hydrochlorides to rats. The purpose of this study was to examine the effect of chemical form, route of administration and vehicle on 3,5‐dichloroaniline‐induced nephrotoxicity. In one set of studies, male Fischer 344 rats (four to eight per group) were administered a single i.p. injection of 3,5‐dichloroaniline free base or hydrochloride salt, cysteine hydrochloride or ornithine hydrochloride (0.8, 1.0 or 1.5 mmol kg−1) or an appropriate vehicle and renal function monitored for 48 h. Only 3,5‐dichloroaniline hydrochloride induced nephrotoxicity that was characterized as acute renal failure. When 3,5‐dichloroaniline free base (0.8 mmol kg−1) was administered in dimethyl sulfoxide (DMSO), all rats died within 24 h. In a second experiment, the free base or hydrochloride form of 3,5‐dichloroaniline (1.5 mmol kg−1) or vehicle (0.9 saline or sesame oil, respectively) were administered orally and renal function monitored for 48 h. No evidence of nephrotoxicity was observed following either treatment. However, when the hydrochloride salt was given in 25 DMSO in 0.9 saline, all rats died within 24 h, with two rats demonstrating increased proteinuria, glucosuria and hematuria within the first 6 h after treatment. These results demonstrate that 3,5‐dichloraniline nephrotoxicity is potentiated by the administration of systemic acid, but that acid alone has no effect on renal function at the dose tested. Also, 3,5‐dichloroaniline (hydrochloride or free base form) is less toxic orally than when administered i.p. In addition, when DMSO is used as part of the vehicle, 3,5‐dichloroaniline toxicity is potentiated. Thus, chemical form, route of administration and vehicle are all important factors in 3,5‐dichlor

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