Development of a general method of limited sampling for the determination of AUC for a drug that displays two-compartment pharmacokinetics

It has been shown previously that it is impossible to measure the volume of distribution at steady state conclusively for a multicompartment system from an iv bolus dose only. The problem lies in deciding from which compartment elimination of the drug occurs in the compartmental model. In this paper

A limited sampling model has been developed for ¯unarizine following a 30 mg oral dose in epileptic patients who were receiving phenytoin or carbamazepine or both, to estimate the area under the curve (AUC) and maximum plasma concentration (C max ). The model was developed using training data sets f

## Abstract A simple, sensitive and reproducible high‐performance liquid chromatographic method for detecting and quantifying saquinavir in human plasma is described. Verapamil was used as internal standard. The method employes a single liquid–liquid extraction step with __tert__‐butil methyl ether