Design synthesis and biological evaluation of compounds for the treatment of alzheimers disease
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Abstract
Alzheimer s dementia is a major cause of disability and mortality. The typical
newlineneuropathological hallmarks are deposition of protein aggregates or plaques,
newlineformation of neurofibrillary tangles and neuronal cell death. Alzheimer s disease
newline(AD) is a complex neurological condition where several genes act independently/in
newlinecoordination with each other and/or with environmental agents. The role of
newlinesulphonamide functional moiety in design of anti-AD agents is well supported by
newlinevarious research groups. Some of the successfully evaluated includes Nacylsulfonamides, N-benzylisatin sulfonamide analogues, and N-aryl sulfonamide
newlinesubstituted 3-morpholino arecoline derivatives with selectivity for reducing Aand#946;
newlineaggregation. A recent example is Verubecestat prepared by Cu-catalyzed C-N
newlinecoupling as well as diastereoselective Mannich type reaction.
newlineThe present work aims to provide a possible solution for AD. In view of this,
newlinea series of substituted aryl sulfonamide derivatives was developed using computeraided drug design methods such as quantitative structure-activity relationship
newline(QSAR) and molecular docking. Series of N-(5-chloro-2-hydroxymethyl)-N-alkylarylsulfonamides was used to develop QSAR models. The molecular level
newlineinteractions of substituted arylsulfonamides towards and#947;-secretase and human AChE
newlinewere studied using AutoDock4.0 using reported docking protocol. Selected
newlinecompounds were synthesized and characterized. During biological evaluation,
newlineinitially acute toxicity studies were performed. The synthesized compounds were
newlineevaluated for their effect on acquisition in scopolamine induced anterograde amnesia
newlineand neuroprotective activity. Behavioural assessment was carried out using Morris
newlineWater Maze (MWM) test and effect on spatial and temporal memory was recorded.
newlineAfter the MWM treatment period, group showing significant results were sacrificed
newlineby decapitation under mild anaesthesia and brains were immediately isolated,
newlineprocessed for performing biochemical assays like lipid peroxidation (LPO), reduced
newlineglutathione (GSH), and AChE