Structural Basis of Drug Recognition by Human Serum Albumin

Background: Human serum albumin (HSA), the most abundant protein in plasma, is a monomeric multi-domain macromolecule with at least nine binding sites for endogenous and exogenous ligands. HSA displays an extraordinary ligand binding capacity as a depot and carrier for many compounds including most acidic drugs. Consequently, HSA has the potential to influence the pharmacokinetics and pharmacodynamics of drugs. Objective: In this review, the structural determinants of drug binding to the multiple sites of HSA are analyzed and discussed in detail. Moreover, insight into the allosteric and competitive mechanisms underpinning drug recognition, delivery, and efficacy are analyzed and discussed. Conclusion: As several factors can modulate drug binding to HSA (e.g., concurrent administration of drugs competing for the same binding site, ligand binding to allosteric-coupled clefts, genetic inherited diseases, and post-translational modifications), ligand binding to HSA is relevant not only under physiological conditions, but also in the pharmacological therapy management.

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Structural Basis of the Drug-binding Specificity of Human Serum Albumin

Journal of Molecular Biology ◽

10.1016/j.jmb.2005.07.075 ◽

2005 ◽

Vol 353 (1) ◽

pp. 38-52 ◽

Cited By ~ 1121

Author(s):

Jamie Ghuman ◽

Patricia A. Zunszain ◽

Isabelle Petitpas ◽

Ananyo A. Bhattacharya ◽

Masaki Otagiri ◽

...

Keyword(s):

Human Serum Albumin ◽

Serum Albumin ◽

Human Serum ◽

Binding Specificity ◽

Drug Binding ◽

Structural Basis

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Exploring the Drug-Binding Site Sudlow I of Human Serum Albumin: The Role of Water and Trp214 in Molecular Recognition and Ligand Binding

ChemPhysChem ◽

10.1002/cphc.201000742 ◽

2010 ◽

Vol 12 (2) ◽

pp. 270-274 ◽

Cited By ~ 41

Author(s):

Osama K. Abou-Zied ◽

Najla Al-Lawatia

Keyword(s):

Human Serum Albumin ◽

Molecular Recognition ◽

Ligand Binding ◽

Serum Albumin ◽

Human Serum ◽

Binding Site ◽

Drug Binding ◽

Drug Binding Site

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The Influence of Oxidative Stress on Serum Albumin Structure as a Carrier of Selected Diazaphenothiazine with Potential Anticancer Activity

Pharmaceuticals ◽

10.3390/ph14030285 ◽

2021 ◽

Vol 14 (3) ◽

pp. 285

Author(s):

Małgorzata Maciążek-Jurczyk ◽

Beata Morak-Młodawska ◽

Małgorzata Jeleń ◽

Wiktoria Kopeć ◽

Agnieszka Szkudlarek ◽

...

Keyword(s):

Human Serum Albumin ◽

Serum Albumin ◽

Human Serum ◽

Anticancer Activity ◽

Drug Distribution ◽

Cd Spectroscopy ◽

Drug Binding ◽

Protein Activity ◽

Chloramine T ◽

The Stability

Albumin is one of the most important proteins in human blood. Among its multiple functions, drug binding is crucial in terms of drug distribution in human body. This protein undergoes many modifications that are certain to influence protein activity and affect its structure. One such reaction is albumin oxidation. Chloramine T is a strong oxidant. Solutions of human serum albumin, both non-modified and modified by chloramine T, were examined with the use of fluorescence, absorption and circular dichroism (CD) spectroscopy. 10H-3,6-diazaphenothiazine (DAPT) has anticancer activity and it has been studied for the first time in terms of binding with human serum albumin—its potential as a transporting protein. Using fluorescence spectroscopy, in the presence of dansylated amino acids, dansyl-l-glutamine (dGlu), dansyl-l-proline (dPro), DAPT binding with two main albumin sites—in subdomain IIA and IIIA—has been evaluated. Based on the conducted data, in order to measure the stability of DAPT complexes with human (HSA) and oxidized (oHSA) serum albumin, association constant (Ka) for ligand-HSA and ligand-oHSA complexes were calculated. It has been presumed that oxidation is not an important issue in terms of 10H-3,6-diazaphenothiazine binding to albumin. It means that the distribution of this substance is similar regardless of changes in albumin structure caused by oxidation, natural occurring in the organism.

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