Selected Class of Enamides Bearing Nitro Functionality as Dual-Acting with Highly Selective Monoamine Oxidase-B and BACE1 Inhibitors

A small series of nitro group-bearing enamides was designed, synthesized (NEA1-NEA5), and evaluated for their inhibitory profiles of monoamine oxidases (MAOs) and beta-site amyloid precursor protein cleaving enzyme 1 (beta-secretase, BACE1). Compounds NEA3 and NEA1 exhibited a more potent MAO-B inhi...

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Veröffentlicht in:Molecules (Basel, Switzerland) Switzerland), 2021-10, Vol.26 (19), p.6004, Article 6004
Hauptverfasser: Venkidath, Anusree, Oh, Jong Min, Dev, Sanal, Amin, Elham, Rasheed, Shebina P., Vengamthodi, Ajeesh, Gambacorta, Nicola, Khames, Ahmed, Abdelgawad, Mohamed A., George, Ginson, Nicolotti, Orazio, Kim, Hoon, Mathew, Bijo
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Sprache:eng
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Zusammenfassung:A small series of nitro group-bearing enamides was designed, synthesized (NEA1-NEA5), and evaluated for their inhibitory profiles of monoamine oxidases (MAOs) and beta-site amyloid precursor protein cleaving enzyme 1 (beta-secretase, BACE1). Compounds NEA3 and NEA1 exhibited a more potent MAO-B inhibition (IC50 value = 0.0092 and 0.016 mu M, respectively) than the standards (IC50 value = 0.11 and 0.14 mu M, respectively, for lazabemide and pargyline). Moreover, NEA3 and NEA1 showed greater selectivity index (SI) values toward MAO-B over MAO-A (SI of > 1652.2 and > 2500.0, respectively). The inhibition and kinetics studies suggested that NEA3 and NEA1 are reversible and competitive inhibitors with K-i values of 0.013 & PLUSMN; 0.005 and 0.0049 & PLUSMN; 0.0002 mu M, respectively, for MAO-B. In addition, both NEA3 and NEA1 showed efficient BACE1 inhibitions with IC50 values of 8.02 & PLUSMN; 0.13 and 8.21 & PLUSMN; 0.03 mu M better than the standard quercetin value (13.40 & PLUSMN; 0.04 mu M). The parallel artificial membrane permeability assay (PAMPA) method demonstrated that all the synthesized derivatives can cross the blood-brain barrier (BBB) successfully. Docking analyses were performed by employing an induced-fit docking approach in the GLIDE module of Schrodinger, and the results were in agreement with their in vitro inhibitory activities. The present study resulted in the discovery of potent dual inhibitors toward MAO-B and BACE1, and these lead compounds can be fruitfully explored for the generation of newer, clinically active agents for the treatment of neurodegenerative disorders.
ISSN:1420-3049
1420-3049
DOI:10.3390/molecules26196004