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Abstract
δ-Aminolevulinic acid dehydratase (δ-ALAD) is a metalloprotein that catalyzes porphobilinogen formation. This enzyme is sensitive to pro-oxidants and classically used as a biomarker of lead (Pb) intoxication. Diphenyl diselenide [(PhSe)2] and analogs bis(4-chlorophenyl) diselenide [(pCl3PhSe)2], bis(4-methoxyphenyl)diselenide [(pCH3OPhSe)2], and bis[3-(trifluoromethy)phenyl] diselenide [(mCF3PhSe)2] inhibit mammalian δ-ALAD by oxidizing enzyme cysteinyl residues, which are involved in diselenide-induced toxicity. 2-Cysteinyl residues from δ-ALAD are believed to sequentially interact with (PhSe)2. Thus this study utilized protein–ligand docking analyses to determine which cysteinyl residues might be involved in the inhibitory effect of (PhSe)2 and analogs toward δ-ALAD. All diselenides that interact in a similar manner with the active site of δ-ALAD were examined. Docking simulations indicated an important role for π–π interactions involving Phe208 and cation–π interactions involving Lys199 and Arg209 residues with the aromatic ring of (PhSe)2 and analogs. Based upon these interactions an approximation between Se atoms and –SH of Cys124, with distances ranging between 3.3 Å and 3.5 Å, was obtained. These data support our previous postulations regarding the mechanism underlying δ-ALAD oxidation mediated by (PhSe)2 and analogs. Based on protein–ligand docking analyses, data indicated that –SH of Cys124 attacks one of the Se atoms of –SH of (PhSe)2 releasing one PhSeH (selenophenol). Subsequently, the –SH of Cys132 attacks the sulfur atom of Cys124 (from the bond of E-S-Se-Ph indermediate), generating the second PhSe–, and the oxidized and inhibited δ-ALAD. In conclusion, AutoDock Vina 1.1.1 was a useful tool to search for diselenides inhibitors of δ-ALAD, and, most importantly, it provided insight into molecular mechanisms involved in enzyme inhibition.
Acknowledgments
We are thankful to CNPq (process no. 142611/2009-3), CAPES VITAE, FINEP, INCT-CNPQ for Excitoxicity and Neuroprotection, FAPERGS-PRONEX-CNPq, and IBNet-FINEP for providing financial support and fellowship to researchers, and to Scripps Research Institute and Accelrys, Inc., for providing free academic license of programs used in this study.