Blind Dockings of Benzothiazoles to Multiple Receptor Conformations of Triosephosphate Isomerase from Trypanosoma cruzi and Human
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Date
2011
Authors
Kurkcuoglu, Zeynep
Ural, Gulgun
Akten, Ebru Demet
Doruker, Pemra
Journal Title
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Volume Title
Publisher
Wiley-VCH Verlag GmbH
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Abstract
We aim to uncover the binding modes of benzothiazoles which have been reported as specific inhibitors of triosephosphate isomerase from the parasite Trypanosoma cruzi (TcTIM) by performing blind dockings on both TcTIM and human TIM (hTIM). Detailed analysis of binding sites and specific interactions are carried out based on ensemble dockings to multiple receptor conformers obtained from molecular dynamics simulations. In TcTIM dimer dockings the inhibitors preferentially bind to the tunnel-shaped cavity formed at the interface of the subunits whereas non-inhibitors mostly choose other sites. In contrast TcTIM monomer binding interface and hTIM dimer interface do not present a specific binding site for the inhibitors. These findings point to the importance of the tunnel and of the dimeric form for inhibition of TcTIM. Specific interactions of the inhibitors and their sulfonate-free derivatives with the receptor residues indicate the significance of sulfonate group for binding affinity and positioning on the TcTIM dimer interface. One of the inhibitors also binds to the active site which may explain its relatively higher inhibition effect on hTIM.
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Keywords
Blind docking, Triosephosphate isomerase, Trypanosoma cruzi, Molecular dynamics, Benzothiazole
Turkish CoHE Thesis Center URL
Fields of Science
Citation
12
WoS Q
Q2
Scopus Q
Q2
Source
Volume
30
Issue
Start Page
986
End Page
995