Background : Metoprolol, the selective ${eta}_1$-adrenoceptor antagonist, is eliminated primarily by hepatic metabolism. Usually less than 5% of an oral dose is excreted unchanged in the urine. Metoprolol is a highly extracted drug and its ${alpha}$-hydroxylation pathway is mediated by CYP2D6. Therefore, it is often used as a probe drug to measure the metabolic capacity of liver. Method : The effects of impaired liver function on the pharmacokinetics of metoprolol were studied in 16 patients with hepatic cirrhosis (modified Child-Pugh class B and C group : 9 and 7 persons, respectively) together with 8 healthy volunteers. Pharmacokinetic parameters in these patients were compared to those in normal subjects. All subjects were given single oral doses of 50mg in the morning fasting state. Blood and urine samples were collected serially. The concentrations of metoprolol and ${alpha}$-OH metoprolol in the biological fluids were measured by high-performance liquid chromatography using fluorescence detector. Results : There were statistically significant differences in $C_{max},;T_{max},;t_{1/2{eta}}$, and $AUC_{0-12hr}$ of metoprolol between the patients and the normal subjects (p<0.05), ${alpha}$-OH metoprolol produced by CYP2D6 was also measured and significant differences in both $C_{max}$ and $T_{max}$ were observed. There was no statistically significant difference in pharmacokinetic parameters between modified Child-pugh class B and C groups. Conclusion : For the sake of safety, the reasonable initial dose of metoprolol for the patients with portocaval shunts or advanced liver disease would be about one third of the usual dose, although the potential for adverse reactions is tempered by the flat dose response curve and the wide therapeutic index of this drug.