Litcius/Paper detail

Three to Tango: Inhibitory Effect of Quercetin and Apigenin on Acetylcholinesterase, Amyloid-β Aggregation and Acetylcholinesterase-Amyloid Interaction

Irene Álvarez-Berbel, Alba Espargaró, Antonio Viayna, Ana B. Caballero, Maria Antònia Busquets, Patrick Gámez, F. Javier Luque, Raimon Sabaté

2022Pharmaceutics33 citationsDOIOpen Access PDF

Abstract

One of the pathological hallmarks of Alzheimer's disease (AD) is the formation of amyloid-β plaques. Since acetylcholinesterase (AChE) promotes the formation of such plaques, the inhibition of this enzyme could slow down the progression of amyloid-β aggregation, hence being complementary to the palliative treatment of cholinergic decline. Antiaggregation assays performed for apigenin and quercetin, which are polyphenolic compounds that exhibit inhibitory properties against the formation of amyloid plaques, reveal distinct inhibitory effects of these compounds on Aβ40 aggregation in the presence and absence of AChE. Furthermore, the analysis of the amyloid fibers formed in the presence of these flavonoids suggests that the Aβ40 aggregates present different quaternary structures, viz., smaller molecular assemblies are generated. In agreement with a noncompetitive inhibition of AChE, molecular modeling studies indicate that these effects may be due to the binding of apigenin and quercetin at the peripheral binding site of AChE. Since apigenin and quercetin can also reduce the generation of reactive oxygen species, the data achieved suggest that multitarget catechol-type compounds may be used for the simultaneous treatment of various biological hallmarks of AD.

Topics & Concepts

ApigeninAcetylcholinesteraseChemistryQuercetinBiochemistryAchéAmyloid (mycology)Inhibitory postsynaptic potentialCholinergicPharmacologyEnzymeBiophysicsFlavonoidAntioxidantBiologyEndocrinologyInorganic chemistryCholinesterase and Neurodegenerative DiseasesComputational Drug Discovery MethodsAlzheimer's disease research and treatments