| dc.description.abstract | The first part of the thesis deals with the structural studies of N-Methyl-D-Aspartate
receptors (NMDARs). NMDARs are ionotropic ligand-gated receptors that have
pivotal roles at the central neuronal system but, hyperactivity of NMDARs could
contribute to neurodegenerative diseases. Therefore, understanding the activation
mechanism of NMDARs is important as it may lead to the development of new
treatments for neurodegenerative diseases.
In this thesis, human GluN1/GluN2A type NMDAR is modeled based on
GluN1/GluN2B type NMDA structures that were resolved in 2014. To observe the
dynamics of NMDA, 1.3 microseconds molecular dynamics simulations are
performed for ligand-free and ligand-bound structures in the physiological
environment. RMSD, RMSF, and PCA have been used to analyze the trajectory
to understand the di↵erences in ligand-free and ligand-bound structures collective
motions.
From these analyses, the di↵erences in between ligand-free and ligand-bound
simulations can be summarized as the following: Ligand-binding domain closure is
observed, and these rearrangements are reflected to the transmembrane linkers
upon ligand binding. Correlation maps from PCA analysis display more correlated
motions in ligand-bound simulations. As a summary, mainly ligands act like an
adhesive for the binding-domain by bringing the bi-lobe structures together and
consequently, this is reflected in the overall dynamics of the protein.
In the second part of this thesis, Xanthine Oxidase (XO) enzyme has been studied
for the potency of bis-chalcones compounds. 8 bis-chalcones compounds that were provided to us from Serdar Burmalıo˘glu’s research group, showed high inhibition
behavior on XO. These 8 molecules are docked to XO catalytic unit and 1000 run is
performed for each compound. All compounds show better results than its approved
drug which is allopurinol, however, the best ones are fifth and seventh compounds.
In addition, all these compounds have three similar binding modes but, the first
pose has the lowest free binding energy | en_US |
