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二氯甲烷代谢及亚慢性经口毒性研究综述,作为大鼠和小鼠慢性经口研究设计的基础。

Review of investigations of dichloromethane metabolism and subchronic oral toxicity as the basis for the design of chronic oral studies in rats and mice.

作者信息

Kirschman J C, Brown N M, Coots R H, Morgareidge K

出版信息

Food Chem Toxicol. 1986 Sep;24(9):943-9. doi: 10.1016/0278-6915(86)90322-4.

Abstract

In preparation for the design and performance of chronic toxicity and carcinogenicity studies in rats and mice on dichloromethane (methylene chloride; DCM), biochemical, mutagenicity, short-term, metabolic and subchronic feeding studies were carried out. These studies established that it was feasible to present DCM to rodents at adequate levels in drinking-water. Saturation of metabolic pathways was demonstrated in both rats and mice at oral doses of approximately 100 mg/kg. The lowest toxic effect levels after 90 days of treatment were found to be approximately 190 and 580 mg/kg for rats and mice, respectively. Dose, vehicle and the exposure regimen were found to affect DCM challenge to target tissues and its metabolism to CO and CO2.

摘要

为了对二氯甲烷(二氯甲烷;DCM)进行大鼠和小鼠的慢性毒性及致癌性研究的设计和实施,开展了生化、致突变性、短期、代谢和亚慢性喂养研究。这些研究表明,以适当水平通过饮用水向啮齿动物提供DCM是可行的。在大鼠和小鼠中,口服剂量约为100mg/kg时均证明代谢途径达到饱和。治疗90天后,大鼠和小鼠的最低毒性作用水平分别约为190mg/kg和580mg/kg。发现剂量、赋形剂和暴露方案会影响DCM对靶组织的攻击及其代谢为CO和CO2的过程。

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