| Title : Liver damage induced in rats by malathion impurities - Keadtisuke_1990_Toxicol.Lett_52_35 |
| Author(s) : Keadtisuke S , Dheranetra W , Nakatsugawa T , Fukuto TR |
| Ref : Toxicol Lett , 52 :35 , 1990 |
|
Abstract :
Administration of a single oral dose of the malathion impurity, O,O,S-trimethyl phosphorothioate (OOS-Me) or O,S,S-trimethyl phosphorodithioate (OSS-Me), to the rat resulted in hemostatic disorders, e.g. prolongation of blood clotting, prothrombin and thrombin time. Deficiency of coagulation Factors II, V and VII was also observed. OOS-Me and OSS-Me also caused dose-dependent increases of beta-glucuronidase in the blood with a maximum of 15- and 31-fold observed following treatment with 60 mg/kg OOS-Me and 40 mg/kg OSS-Me, respectively. Analysis of serum beta-glucuronidase by isoelectrofocusing electrophoresis showed that the liver endoplasmic reticulum was the source of this enzyme released into the blood. Co-treatment of OOS-Me with 5% O,O,O-trimethyl phosphorothioate (OOO-Me), a potent antagonist of OOS-Me-induced delayed toxicity, prevented hemostatic disorders but had no effect in reducing beta-glucuronidase levels. However, pretreatment of rats with piperonyl butoxide reduced the amount of beta-glucuronidase released into the blood. Of other O,O,S-trialkyl phosphorothioates examined, the O,O-diethyl S-alkyl phosphorothioates showed the highest activity in increasing beta-glucuronidase levels. |
| PubMedSearch : Keadtisuke_1990_Toxicol.Lett_52_35 |
| PubMedID: 2356569 |
Keadtisuke S, Dheranetra W, Nakatsugawa T, Fukuto TR (1990)
Liver damage induced in rats by malathion impurities
Toxicol Lett
52 :35
Keadtisuke S, Dheranetra W, Nakatsugawa T, Fukuto TR (1990)
Toxicol Lett
52 :35