Development of a Minimally Invasive Protocol for the Determination of Phenylalanine and Lysine Kinetics in Humans during the Fed State

Abstract

The primed, continuous intravenous infusion of amino acids labeled with ¹³C together with measurement of isotopic enrichment in plasma is commonly used to study amino acid metabolism. However, a less invasive, oral infusion that also produces an isotopic steady state in CO₂ and urine would be useful, particularly for pediatric studies. We measured the ¹³C enrichments of expired CO₂, plasma and urine free phenylalanine and lysine and estimated flux and oxidation rates in adult humans (n = 12) who received a 4-h oral, primed, equal dose infusion of either L-[1-¹³C]phenylalanine, L-[1-¹³C]lysine (D-lysine = 1.6%) or L-[1-¹³C]lysine (D-lysine ≤ 0.2%). Steady fed state conditions were established by feeding subjects eight hourly meals beginning 4 h before the start of the oral infusion protocol. Isotopic plateau in CO₂, plasma and urine was achieved within 120 min of phenylalanine or lysine infusion. At isotopic plateau, the mean ratio of plasma to urine enrichment was 1.0 ± 0.04 (SEM), 0.39 ± 0.03 and 0.97 ± 0.02 for L-[1-¹³C]phenylalanine, L-[1-¹³C]lysine (D-lysine = 1.6%) and L-[1-¹³C]lysine (D-lysine≤ 0.2%), respectively. There was good agreement between isotopic enrichment in plasma and urine for L-[1-¹³C]phenylalanine and L-[1-¹³C]lysine (D-lysine ≤ 0.2%). However, use of L-[1-¹³C]lysine (D-lysine = 1.6%) resulted in significantly higher enrichment in urine, probably due to renal tubular discrimination of D-lysine. Mean flux rates for phenylalanine and lysine were consistent with the literature. Thus, the oral, primed, equal dose infusion produces the isotopic steady-state condition required for amino acid flux and oxidation determination within an 8-h period.