Litcius/Paper detail

Whole Blood Or Plasma: What is the Ideal Matrix for pharmacokinetic-driven Drug Candidate selection?

Ranjeet Prasad Dash, Vijayabhaskar Veeravalli, Jennifer A. Thomas, Clint Rosenfeld, Nirali Mehta, Nuggehally R. Srinivas

2020Future Medicinal Chemistry32 citationsDOI

Abstract

In the present era of drug development, quantification of drug concentrations following pharmacokinetic studies has preferentially been performed using plasma as a matrix rather than whole blood. However, it is critical to realize the difference between measuring drug concentrations in blood versus plasma and the consequences thereof. Pharmacokinetics using plasma data may be misleading if concentrations differ between plasma and red blood cells (RBCs) because of differential binding in blood. In this review, factors modulating the partitioning of drugs into RBCs are discussed and the importance of determining RBC uptake of drugs for drug candidate selection is explored. In summary, the choice of matrix (plasma vs whole blood) is an important consideration to be factored in during drug discovery.

Topics & Concepts

PharmacokineticsDrugPharmacologyWhole bloodBlood plasmaDrug discoveryMatrix (chemical analysis)ChemistryPlasma concentrationMedicineChromatographyInternal medicineBiochemistryDrug Transport and Resistance MechanismsBlood groups and transfusionAntibiotics Pharmacokinetics and Efficacy