Planejamento, síntese e avaliação da atividade anticolinesterásica de análogos de Piperina
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Universidade Estadual de Goiás
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Abstract
Alzheimer's disease (AD) is a chronic neurodegenerative disorder characterized by
progressive and irreversible loss of memory and cognitive functions. Is the most
common cause of dementia in elderly people, accounting for about 80% of cases.
Existing treatments are only symptomatic. The more modern drugs act by increasing
acetylcholine levels by inhibiting the enzyme acetylcholinesterase (AChE). However,
their action is not always successful, especially in advanced stages of the disease,
which justifies the search for new inhibitors that are more potent and less severe
adverse effects. For this, the use of molecular modeling techniques as a strategy for
rational drug design is a good bet and various substances of natural origin have been
used as a prototype. The objective of this study was to design and synthesize
compounds with promising acetylcholinesterase from the piperine molecule after
molecular docking simulations. For this, the virtual assays were performed using the
program GOLD 4.1, based on the mode of interaction between donepezil and AChE
due to structural similarity between this drug and piperine. Based on the results of
these preliminary assays it was proposed the synthesis of a series of asymmetric
azines structurally related to the prototype. Forty compounds with different
substitution patterns were synthesized. The anticholinesterase activity of the
substances was evaluated by in vitro microplate assay with Ellman's reagent (Method
modified by Rhee). Among these compounds, 5 showed the ability to inhibit AChE,
albeit with lower percentages of inhibition obtained for the piperine 12, acid 13 and
piperic ester 14 which were: 46.5, 50.6 and 63.6%, respectively. In addition the
antioxidant potential of the substances tested with anticholinesterase activity was
evaluated by voltammetry. Of these, compounds 12, 13, 14, 46 and 47 showed
electroactivity.
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FIGUEREDO, A. S. Planejamento, síntese e avaliação da atividade anticolinesterásica de análogos de Piperina. 2013. 169 f. Dissertação (Mestrado em Ciências Moleculares) - Câmpus Central - Sede: Anápolis – CET, Universidade Estadual de Goiás, Anápolis-GO.
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