Hexachloro-1:3-butadiene-induced renal tubular necrosis in the mouse

## Abstract The effect of a single i.p. dose of 200 or 300 mg kg^−1^ hexachloro‐1:3‐butadiene (HCBD) on liver morphology, water, sodium and potassium ion content, cation movement and non‐protein sulphydryl (NP‐SH) content has been studied in rats. There was a rapid, dose‐related increase in liver w

## Abstract Renal tissue biomarkers (glutamine synthetase and __p__‐aminohippuric acid uptake) were studied in male and female rats after treatment with hexachloro‐1,3‐butadiene. Reduced glutathione content also was also determined in liver and kidney. Histopathological examination (light microscop

Renal, biliary, pulmonary and faecal excretion experiments were carried out with labelled hexachloro-1,3butadiene ([I4C]HCBD) in male Sprague-Dawley rats, given orally (p.0.) and intravenously (i.v.) in doses of 1 and 100 mg kg-' as a solution in polyethylene glycol. The radioactivity excreted over

Male Sprague Dawley rats with cannulated bile duct (BDC rats) received 100 or 200 mg kg-I labelled hexachloro-l,3-butadiene ([I4C]HCBD) by gavage 1 h (BDCI rats) or 24 h (BDCM rats) after surgical cannula implantation. Twenty-four hours after treatment with HCBD, rats were examined histochemically a