Multiple activation of chloroform in hepatic microsomes from uninduced B6C3F1 mice

Microsomes from the renal cortex of DBA/2J mice can metabolize chloroform through oxidative and reductive pathways, similar to hepatic microsomes. The oxidative or reductive nature of CHC13 activation is strictly dependent on the oxygenation of the incubation mixture, as indicated by the formation

## Abstract The oral and i.v. elimination kinetics were investigated for bromodichloroacetate (BDCA), a haloacetate found in drinking water. The BDCA was administered at a dose of 5, 20 and 100 mg kg^−1^ to B6C3F1 mice and appears to distribute to the total body water with a mean volume of distribu

The weight of evidence indicates that chloroform then held until analysis 10, 30, 90, and 180 days induces cancer in the female B6C3F 1 mouse liver postexposure. Livers from DMN-treated mice exhibvia a nongenotoxic-cytotoxic mode of action. How-ited a dose-related 2-to 5-fold increase over control e