Discovery of N-(1-(3-fluorobenzoyl)-1H-indol-5-yl)pyrazine-2-carboxamide: a novel, selective, and competitive indole-based lead inhibitor for human monoamine oxidase B

Authors
Elkamhawy, AhmedPaik, SoraKim, Hyeon JeongPark, Jong-HyunLondhe, Ashwini M.Lee, KyeongPae, Ae NimPark, Ki DukRoh, Eun Joo
Issue Date
2020-01
Publisher
Taylor & Francis
Citation
Journal of Enzyme Inhibition and Medicinal Chemistry, v.35, no.1, pp.1568 - 1580
Abstract
Herein, two new series ofN-substituted indole-based analogues were rationally designed, synthesizedviamicrowave heating technology, and evaluated as noteworthy MAO-B potential inhibitors. Compared to the reported indazole-based hitsVIandVII, compounds4band4eexhibited higher inhibitory activities over MAO-B with IC(50)values of 1.65 and 0.78 mu M, respectively. When compared to the modest selectivity index of rasagiline (II, a well-known MAO-B inhibitor, SI > 50), both4band4ealso showed better selectivity indices (SI > 60 and 120, respectively). A further kinetic evaluation of the most potent derivative (4e) displayed a competitive mode of inhibition (inhibition constant (K-i)/MAO-B = 94.52 nM). Reasonable explanations of the elicited biological activities were presentedviaSAR study and molecular docking simulation. Accordingly, the remarkable MAO-B inhibitory activity of4e(N-(1-(3-fluorobenzoyl)-1H-indol-5-yl)pyrazine-2-carboxamide), with its selectivity and competitive inhibition, advocates its potential role as a promising lead worthy of further optimization.
Keywords
PARKINSONS-DISEASE; DERIVATIVES; SAFINAMIDE; TARGETS; OPTIMIZATION; SEMBRAGILINE; PHARMACOLOGY; MODELS; POTENT; Monoamine oxidase B; carboxamide; MAO-B inhibitor; microwave synthesis; molecular modelling
ISSN
1475-6366
URI
https://pubs.kist.re.kr/handle/201004/119128
DOI
10.1080/14756366.2020.1800666
Appears in Collections:
KIST Article > 2020
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