Influence of the defective metabolism of sparteine on its pharmacokinetics

Abstract

Sparteine is metabolized by N₁-oxidation, which in some subjects is defective. The defect has a pronounced effect on the kinetics of the drug. In non-metabolisers elimination of sparteine proceeds entirely via renal excretion by a capacity-limited process, 99,9% of the dose being excreted as unchanged drug. In metabolisers the drug is mainly eliminated by metabolic degradation. Pronounced differences in β-phase half-life and total plasma clearance were observed between metabolisers (156 min; 535 ml · min⁻¹) and nonmetabolisers (409 min; 180 ml · min⁻¹).