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Xenobiotica
the fate of foreign compounds in biological systems
Volume 45, 2015 - Issue 10
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General Xenobiochemistry

Characterization of the comparative drug binding to intra- (liver fatty acid binding protein) and extra- (human serum albumin) cellular proteins

, , , , , , & show all
Pages 847-857 | Received 14 Dec 2014, Accepted 17 Feb 2015, Published online: 24 Mar 2015
 

Abstract

1. This study compared the extent, affinity, and kinetics of drug binding to human serum albumin (HSA) and liver fatty acid binding protein (LFABP) using ultrafiltration and surface plasmon resonance (SPR).

2. Binding of basic and neutral drugs to both HSA and LFABP was typically negligible. Binding of acidic drugs ranged from minor (fu > 0.8) to extensive (fu< 0.1). Of the compounds screened, the highest binding to both HSA and LFABP was observed for the acidic drugs torsemide and sulfinpyrazone, and for β-estradiol (a polar, neutral compound).

3. The extent of binding of acidic drugs to HSA was up to 40% greater than binding to LFABP. SPR experiments demonstrated comparable kinetics and affinity for the binding of representative acidic drugs (naproxen, sulfinpyrazone, and torsemide) to HSA and LFABP.

4. Simulations based on in vitro kinetic constants derived from SPR experiments and a rapid equilibrium model were undertaken to examine the impact of binding characteristics on compartmental drug distribution. Simulations provided mechanistic confirmation that equilibration of intracellular unbound drug with the extracellular unbound drug is attained rapidly in the absence of active transport mechanisms for drugs bound moderately or extensively to HSA and LFABP.

Acknowledgements

Technical assistance from Mr DJ Elliot and Dr BC Lewis is gratefully acknowledged.

Declaration of interest

The authors report that they have no conflicts of interest. This work was funded, in part, by a project grant from the National Health and Medical Research Council of Australia [Grant ID 595920].

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