3D-QSAR with CoMFA Model of Prolylendopeptidase Substrates |
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| Authors: | A. V. Veselovsky E. G. Matveeva N. N. Zolotov A. S. Ivanov |
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| Affiliation: | Institute of Biomedical Chemistry RAMS , Moscow, Russia |
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| Abstract: | ![]()
Abstract The prolylendopeptidase (PEP) is the proteolytic enzyme, which plays an essential role in the regulation of some processes in central nervous system, such as memory, learning and behavior. It was shown that PEP activity changes at different diseases, like Parkinsons or Alzheimer's diseases, and some PEP inhibitors are used in therapy. At present time the discovery of new types of PEP inhibitors are the actual task. In this study the structure of PEP active site was analyzed by 3D-QSAR with CoMFA methods using of 12 PEP substrates. The designed pharmacophore model assumes that substrates interact with PEP active site by pyrrolidol ring of proline residue and by hydrogen bonding. The 3-D-QSAR + CoMFA model of PEP substrates propose that the hydrophobic bonds play the essential role in substrate interaction with enzyme. This model reveals the important steric and electrostatic areas around the molecules and the presence of substituents controls the PEP activity for substrates. Analysis of obtained data allows to assume, that substrate binding in PEP active site causes essential perturbations of substrate structure. This effect mainly depends on chemical nature of the amino acid side chain, located near to proline. |
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| Keywords: | Prolylendopeptidase 3D-QSAR CoMFA pharmacophore active site substrate |
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