Hypoxia and CCI 4 ‐induced liver injury, but not acidosis, impair metabolism of cysteinyl leukotrienes in perfused rat liver

Uptake, metabolism and biliary elimination of infused cysteinyl leukotrienes were investigated in single‐pass perfused rat liver. Hypoxia did not impair uptake of infused [ 3 H] leukotriene C 4 , but inhibited biliary excretion of radioactivity by about 50% compared with normoxic control experiments. In addition, the leukotriene metabolite pattern in bile was profoundly altered and was characterized in hypoxia by a 75% to 80% decrease of both leukotriene C 4 and polar metabolites, representing ω‐oxidation products, whereas the appearance of leukotriene D 4 in bile was not affected. Reoxygenation was followed by a marked increase of biliary excretion of polar metabolites, indicating that leukotrienes taken up and stored in the liver cells during the hypoxic period now underwent ω‐oxidation with subsequent slimination of the ω‐oxidized products. Hypoxia also inhibited the biliary excretion of radioactivity after [ 3 H] leukotriene E 4 addition because of an almost complete absence of ω‐oxidation products in bile, whereas N‐acetylleukotriene E 4 excretion was not affected. Induction of liver injury by carbon tetrachloride treatment decreased single‐pass uptake of [ 3 H] leukotriene C 4 by 30%, and only 36% of the radioactivity taken up by the liver was eliminated into bile within 1 hr, compared with 78% in normal livers. The pattern of biliary leukotriene metabolites, however, was not significantly different. Lowering the pH in the perfusion medium from 7.4 to 7.1 had no effect on uptake, metabolism or biliary elimination of infused [ 3 H] leukotriene C 4 . The data show that hypoxia and experimental liver injury, but not acidosis, impair hepatic processing of cysteinyl leukotriences. Thus, in leukotriene‐induced shock syndromes, leukotriene elimination and inactivation may be imnpaired giving rise to a “vicious circle.”(HEPATOLOGY 1990; 11:866‐873.)