Molecular docking of thiamine reveals similarity in binding properties between the prion protein and other thiamine-binding proteins

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DOIResolve DOI: http://doi.org/10.1007/s00894-013-1979-5
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TypeArticle
Journal titleJournal of Molecular Modeling
ISSN1610-2940
Volume19
Issue12
Pages52255235; # of pages: 11
Subjectligand; phosphate; prion protein; thiamine; tyrosine; water interaction; hydrogen bond; molecular docking; mutation; nuclear magnetic resonance; Pi stacking; protein binding; X ray crystallography
AbstractPrion-induced diseases are a global health concern. The lack of effective therapy and 100 % mortality rates for such diseases have made the prion protein an important target for drug discovery. Previous NMR experimental work revealed that thiamine and its derivatives bind the prion protein in a pocket near the N-terminal loop of helix 1, and conserved intermolecular interactions were noted between thiamine and other thiamine-binding proteins. Furthermore, water-mediated interactions were observed in all of the X-ray crystallographic structures of thiamine-binding proteins, but were not observed in the thiamine-prion NMR study. To better understand the potential role of water in thiamine-prion binding, a docking study was employed using structural X-ray solvent. Before energy minimization, docked thiamine assumed a "V" shape similar to some of the known thiamine-dependent proteins. Following minimization with NMR-derived restraints, the "F" conformation was observed. Our findings confirmed that water is involved in ligand stabilization and phosphate group interaction. The resulting refined structure of thiamine bound to the prion protein allowed the 4-aminopyrimidine ring of thiamine to π-stack with Tyr150, and facilitated hydrogen bonding between Asp147 and the amino group of 4-aminopyrimidine. Investigation of the π-stacking interaction through mutation of the tyrosine residue further revealed its importance in ligand placement. The resulting refined structure is in good agreement with previous experimental restraints, and is consistent with the pharmacophore model of thiamine-binding proteins. © 2013 Springer-Verlag Berlin Heidelberg.
Publication date
LanguageEnglish
AffiliationNational Research Council Canada (NRC-CNRC); Security and Disruptive Technologies
Peer reviewedYes
NPARC number21271812
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Record identifier72240a34-5944-403c-a87d-0b6071e7802f
Record created2014-04-22
Record modified2016-05-09
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