DISCRIMINATION BETWEEN THE VENOUS EQUILIBRIUM AND SINUSOIDAL MODELS OF HEPATIC DRUG ELIMINATION IN THE ISOLATED PERFUSED-RAT-LIVER BY PERTURBATION OF PROPRANOLOL PROTEIN-BINDING
- 1 January 1984
- journal article
- research article
- Vol. 229 (2) , 522-526
- https://doi.org/10.1016/s0022-3565(25)21990-5
Abstract
To discriminate between 2 widely used models of hepatic drug elimination, the venous equilibrium and sinusoidal models, the effect of altering perfusate protein binding on the hepatic elimination of the highly cleared drug, propranolol, by the isolated perfused rat liver was studied. The relationship between the unbound fraction of drug perfusing the liver and the steady-state unbound drug concentration in hepatic venous effluent (i.e., in the perfusate reservoir) was studied after a constant infusion of drug (1.37 mg/h) into the portal vein. Each rat liver (n = 21) was perfused over 60 min at 1 of 7 different protein concentrations, such that the unbound fraction of propranolol in the portal venous perfusate was varied from 0.1-0.65. The unbound steady-state propranolol concentration in the hepatic venous effluent remained unchanged, despite an almost 7-fold increase in the free fraction of propranolol perfusing the liver. The data conform precisely to the predictions of the venous equilibrium model and are incompatible with the sinusoidal model, which predicts a 100-fold decrease in unbound reservoir concentration. Evidently the apparently unphysiological venous equilibrium model represents a valid description of the hpeatic elimination of this high clearance compound.This publication has 16 references indexed in Scilit:
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