Ontogenic aspects of liver and kidney catechol‐O‐ methyltransferase sensitivity to tolcapone

Abstract

1 The present work describes the catechol-O-methyltransferase (COMT) activities in the liver and kidney of developing and adult rats (aged 3, 6, 9, 18, 30 and 60 days; n = 5 per group) and evaluates the enzyme sensitivity to inhibition by tolcapone, a reversible COMT inhibitor. 2 COMT activity, evaluated by the ability to methylate adrenaline to metanephrine, was determined in liver and kidney homogenates prepared in 0.5 mM phosphate buffer (pH = 7.8) containing pargyline (0.1 mM), MgC1₂ (0.1 mM), EGTA (1 mM) and S-adenosyl-L-methionine (0.1 mM). V_max (in nmol mg⁻¹ protein h⁻¹) of liver COMT was found to decrease gradually with age, from 5.3±0.5 at the age of 3 days up to 2.9±0.2 at the age of 60 days; for the same age range, K_m values (in μm; geometric means with 95% confidence limits) increased from 3.3 (1.0, 7.5) up to 13.1 (2.1, 24.1). At the age of 3 days, V_max values for kidney COMT (2.6±0.1) were lower than those for the liver COMT. However, V_max values for kidney COMT were found to increase up to 6.2±0.6 at the age of 18 days and then declined by 44% at the age of 30 and 60 days. In kidney, aging was also accompanied by an increase in K_m values for COMT (from 2.7 [1.1, 4.3] up to 24.0 [11.7, 36.3]). 3 The sensitivity of liver and renal COMT activity to tolcapone was markedly dependent on the age, 3-days old rats being more sensitive to tolcapone than older animals. The IC₅₀ values (in nM) for inhibition of liver COMT by tolcapone increased gradually with age, from 41 (26, 65) at the age of 3 days up to 720 (640, 800) at the age of 60 days. As was found in the liver, IC₅₀ values (in nM) for inhibition of kidney COMT by tolcapone also increased with age, from 8 (6, 10) at the age of 3 days up to 177 (131, 240) at the age of 60 days. In all experimental groups, the IC₅₀ values for inhibition of liver COMT by tolcapone was higher than those for kidney COMT. 4 In conclusion, these results suggest that aging is accompanied by a decrease in liver and kidney COMT affinity for the substrate (evidenced by the increase in K_m values) and a decrease in sensivity towards inhibition by tolcapone (evidenced by the increase in IC₅₀ values). Furthermore, kidney COMT is shown to be more sensitive to inhibition by tolcapone than liver COMT, irrespective of the age of the animal.