Some Pitfalls in Selecting Descriptive Pharmacokinetic Models

Author:

Vree Tom B.,Hekster Yechiel A.,Oosterbaan Marijn J.M.,Termond Emiel F.S.

Abstract

Some pitfalls in selecting pharmacokinetic models are enumerated. To calculate the pharmacokinetic parameters of a drug that exhibits a biphasic convex plasma concentration-time curve, a two-compartment model does not automatically have to be applied. When only the parent drug in plasma is considered, a two-compartment model seems to be most appropriate. However, when the kinetic behavior of the metabolite has to be taken into account, and when a metabolic equilibrium underlies the metabolic elimination, the two-compartment model may not be appropriate. Also, when calculating the kinetic parameters of a drug with a concave biphasic plasma concentration-time curve, a capacity-limited metabolic conversion is not the automatic explanation for this observation. Limitations in renal excretion and bioavailability may be the reasons for this behavior. Convex and concave biphasic plasma concentration-time curves are illustrated, using sulfonamides as test compounds.

Publisher

SAGE Publications

Subject

Pharmacology (medical),General Pharmacology, Toxicology and Pharmaceutics

Reference18 articles.

1. PARA-AMINOBENZENESULFONAMIDE

2. Wagner JG. Fundamentals of clinical pharmacokinetics. Hamilton, IL: Drug Intelligence Publications, 1975: 82–90.

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