Effects of cholesterol and model transmembrane proteins on drug partitioning into lipid bilayers as analysed by immobilized-liposome chromatography

Author:

Lagerquist Caroline1,Beigi Farideh1,Karlén Anders2,Lennernäs Hans3,Lundahl Per1

Affiliation:

1. Department of Biochemistry, Uppsala Biomedical Center, Uppsala University, Uppsala, Sweden

2. Department of Organic Pharmaceutical Chemistry, Uppsala Biomedical Center, Uppsala University, Uppsala, Sweden

3. Department of Pharmacy, Uppsala Biomedical Center, Uppsala University, Uppsala, Sweden

Abstract

Abstract We have analysed how cholesterol and transmembrane proteins in phospholipid bilayers modulate drug partitioning into the bilayers. For this purpose we determined the chromatographic retention of drugs on liposomes or proteoliposomes entrapped in gel beads. The drug retention per phospholipid amount (the capacity factor Ks) reflects the drug partitioning. Cholesterol in the bilayers decreased the Ks value and hence the partitioning into the membrane in proportion to the cholesterol fraction. On average this cholesterol effect decreased with increasing temperature. Model transmembrane proteins, the glucose transporter GLUT1 and bacteriorhodopsin, interacted electrostatically with charged drugs to increase or decrease the drug partitioning into the bilayers. Bacteriorhodopsin proteoliposomes containing cholesterol combined the effects of the protein and the cholesterol and approached the partitioning properties of red blood cell membranes. For positively charged drugs the correlation between calculated intestinal permeability and log Ks was fair for both liposomes and bacteriorhodopsin-cholesterol proteoliposomes. Detailed modeling of solute partitioning into biological membranes may require an extensive knowledge of their structures.

Publisher

Oxford University Press (OUP)

Subject

Pharmaceutical Science,Pharmacology

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