THE AMINOPYRINE BREATH TEST AS A MEASURE OF LIVER-FUNCTION - A QUANTITATIVE DESCRIPTION OF ITS METABOLIC BASIS IN NORMAL SUBJECTS

Abstract

The APBT [aminopyrine breath test] is widely used as a measure of liver function. The development of the APBT into a liver function test of greater diagnostic value requires quantitative information on the processes involved in aminopyrine disposition and metabolism in man and on how APBT values reflect changes in these processes. A dual-isotope kinetic study of aminopyrine disposition and metabolism was carried out on 5 normal adult subjects. Oral administration of 13C-aminopyrine (2 mg/kg) accompanied by simultaneous i.v. injection of 14C-aminopyrine was followed by serial measurements of aminopyrine and monomethylaminopyrine in plasma and urine over 6 h. Timed collections of respiratory CO2 were analyzed for the content of excess 13CO2 and for 14CO2. On separate days, an i.v. bolus of 13C-labeled NaHCO3 was administered to obtain estimates of the kinetic parameters of CO2 elimination in each subject. These data were fitted simultaneously to a multicompartmental model that, in addition to providing hitherto unavailable quantitative information, has revealed that demethylation is the major elimination pathway for aminopyrine; a major alternative pathway not involving demethylation exists for monomethylaminopyrine and only 50% of the labeled carbon generated by demethylation eventually is oxidized to HCO3-. The sensitivity of 7 types of APBT scores to 50% reductions in the rates of aminopyrine absorption, metabolism of monomethylaminoantipyrine, intermediate carbon metabolism and bicarbonate kinetics was evaluated with breath test curves simulated using the APBT model. Every APBT score currently in use was affected by variations in both gastrointestinal output of aminopyrine and bicarbonate kinetics. There is a need for further development of selective scoring methods in the aminopyrine breath test.