2016
DOI: 10.3389/fnins.2016.00205
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Multi-Target Directed Donepezil-Like Ligands for Alzheimer's Disease

Abstract: HIGHLIGHTS• ASS234 is a MTDL compound containing a moiety from Donepezil and the propargyl group from the PF 9601N, a potent and selective MAO B inhibitor. This compound is the most advanced anti-Alzheimer agent for preclinical studies identified in our laboratory.• Derived from ASS234 both multipotent donepezil-indolyl (MTDL-1) and donepezil-pyridyl hybrids (MTDL-2) were designed and evaluated as inhibitors of AChE/BuChE and both MAO isoforms. MTDL-2 showed more high affinity toward the four enzymes than MTDL… Show more

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Cited by 126 publications
(88 citation statements)
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References 270 publications
(304 reference statements)
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“…Interestingly, some drug candidates have emerged from MTDL design showing promising multi-target properties and have been submitted to extensive bio-pharmacological profiling (Cavalli et al, 2008). Members of the Cost ACTION CM1103 (http://www.cost.eu/COST_Actions/cmst/CM1103) have designed, synthetized and evaluated new different MTDL compounds acting on ChE and MAO-I that may elicit better outcomes in the complex nature of AD than the current selective drugs (Benek et al, 2015; Ismaili et al, 2016; Unzeta et al, 2016). Moreover, MAO-Is with additional ion-chelating and/or antioxidant activities, compounds with dual MAO-I and adenosine A2aR antagonist activity have been characterized (Pisani et al, 2011; Guzior et al, 2015).…”
Section: Monoaminergic Strategies To Treat Epilepsymentioning
confidence: 99%
“…Interestingly, some drug candidates have emerged from MTDL design showing promising multi-target properties and have been submitted to extensive bio-pharmacological profiling (Cavalli et al, 2008). Members of the Cost ACTION CM1103 (http://www.cost.eu/COST_Actions/cmst/CM1103) have designed, synthetized and evaluated new different MTDL compounds acting on ChE and MAO-I that may elicit better outcomes in the complex nature of AD than the current selective drugs (Benek et al, 2015; Ismaili et al, 2016; Unzeta et al, 2016). Moreover, MAO-Is with additional ion-chelating and/or antioxidant activities, compounds with dual MAO-I and adenosine A2aR antagonist activity have been characterized (Pisani et al, 2011; Guzior et al, 2015).…”
Section: Monoaminergic Strategies To Treat Epilepsymentioning
confidence: 99%
“…Donepezil is well known as a cholinesterase inhibitor that is approved for AD treatment. Donepezil is effective in improving cognitive function [3738]. Furthermore, the Aβ 1-42 -infused rat model that we used here shows the pathological hallmarks of AD, including amyloid deposition, robust neuroinflammation, synaptic marker changes, neuronal death, and memory impairments [2333].…”
Section: Discussionmentioning
confidence: 99%
“…Several libraries of donepezil‐linked hybrids had been reported in which the N ‐benzylpiperidine motif of donepezil was linked to the N ‐propargylamine motif of PF9601N ( 237 ), a potent and selective MAO‐BI with neuroprotective effects via means of different heterocyclic ring systems like indole, pyridine, or 8‐hydroxyquinoline; with special emphasis on compound ASS234 ( 238 ), an N ‐propargylindole derivative (Figure ) . ASS234 { N ‐[5‐(3‐(1‐benzylpiperidin‐4‐yl)propoxy)‐1‐methyl‐1 H ‐indol‐2‐ylmethyl]‐ N ‐methylprop‐2‐yn‐1‐amine} ( 238 ) was developed with a view to combine the anticholinergic property of donepezil with a propargylamine moiety derived from selective MAO‐BI, PF9601N ( 237 ) .…”
Section: Discovery and Development Of Mao‐b Inhibitors (2015‐2018)mentioning
confidence: 99%
“…Donepezil‐linked hybrids ( 237‐242 ) . hMAO, human monoamine oxidase; IC 50 , half maximal inhibitory concentration…”
Section: Discovery and Development Of Mao‐b Inhibitors (2015‐2018)mentioning
confidence: 99%