Computer-aided discovery of novel AMPK activators through virtual screening and SAR-driven synthesis

Jeon, Kyung-Hwa; Shin, Jae-Ho; Jo, Hyun-Ji; Kim, Hyunjeong; Park, Seojeong; Kim, Seojeong; Lee, Juhong; Kim, Eosu; Na, Younghwa; Kwon, Youngjoo

doi:10.1016/j.ejmech.2025.117318

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Computer-aided discovery of novel AMPK activators through virtual screening and SAR-driven synthesis

Authors: Jeon, Kyung-Hwa ; Shin, Jae-Ho ; Jo, Hyun-Ji ; Kim, Hyunjeong ; Park, Seojeong ; Kim, Seojeong ; Lee, Juhong ; Kim, Eosu ; Na, Younghwa ; Kwon, Youngjoo

Citation: EUROPEAN JOURNAL OF MEDICINAL CHEMISTRY, Vol.287, 2025-04

Article Number: 117318

Journal Title: EUROPEAN JOURNAL OF MEDICINAL CHEMISTRY

ISSN: 0223-5234

Issue Date: 2025-04

MeSH: AMP-Activated Protein Kinases* / chemistry ; AMP-Activated Protein Kinases* / metabolism ; Computer-Aided Design ; Dose-Response Relationship, Drug ; Drug Discovery ; Drug Evaluation, Preclinical ; Enzyme Activators / chemical synthesis ; Enzyme Activators / chemistry ; Enzyme Activators / pharmacology ; Humans ; Molecular Docking Simulation* ; Molecular Structure ; Small Molecule Libraries / chemical synthesis ; Small Molecule Libraries / chemistry ; Small Molecule Libraries / pharmacology ; Structure-Activity Relationship

Keywords: Hydroxymethylglutaryl Coenzyme A Reductase Kinase ; Amp-activated Protein Kinases ; Enzyme Activators ; Small Molecule Libraries ; 1 (2,4 Dihydroxyphenyl) 3 [4 (piperidin 1 Yl)phenyl]prop 2 En 1 One ; 1 (3 Aminophenyl) 3 (2,5 Dimethoxyphenyl)prop 2 En 1 One ; 1 (3 Aminophenyl) 3 (4 Hydroxy 2 Methoxyphenyl)prop 2 En 1 One ; 1 (3 Aminophenyl) 3 (4 Methoxyphenyl)prop 2 En 1 One ; 1 (3 Aminophenyl) 3 [4 (piperidin 1 Yl)phenyl]prop 2 En 1 One ; 1 (4 Aminophenyl) 3 (2,4 Dimethoxyphenyl)prop 2 En 1 One ; 1 (4 Aminophenyl) 3 (2,5 Dimethoxyphenyl)prop 2 En 1 One ; 1 (4 Aminophenyl) 3 [4 (piperidin 1 Yl)phenyl]prop 2 En 1 One ; 1 (4 Hydroxyphenyl) 3 [4 (piperidin 1 Yl)phenyl]prop 2 En 1 One ; 3 (4 Hydroxy 2 Methoxyphenyl) 1 [4 (piperazin 1 Yl)phenyl]prop 2 En 1 One ; 3 (4 Hydroxyphenyl) 1 [4 (4 Methylpiperazin 1 Yl)phenyl]prop 2 En 1 One ; 4 Chloro N [(4 Chlorophenyl)sulfonyl] N [3 [3 (2,5 Dimethoxyphenyl)acryloyl]phenyl]benzenesulfonamide ; 4 Chloro N [3 [3 (2,5 Dimethoxyphenyl)acryloyl]phenyl]benzenesulfonamide ; 4 Chloro N [3 [3 (4 Methoxyphenyl)acryloyl]phenyl]benzenesulfonamide ; 4 Chloro N [4 [3 (2,5 Dimethoxyphenyl)acryloyl]phenyl]benzenesulfonamide ; Hydroxymethylglutaryl Coenzyme A Reductase Kinase Activator ; Unclassified Drug ; Enzyme Activator ; Hydroxymethylglutaryl Coenzyme A Reductase Kinase ; Animal Cell ; Article ; Computer Aided Design ; Computer Model ; Controlled Study ; Drug Synthesis ; Enzyme Activation ; Enzyme Activity ; In Vitro Study ; Molecular Docking ; Mouse ; Nonhuman ; Pharmacophore ; Scn2a Cell Line ; Structure Activity Relation ; Chemical Structure ; Chemistry ; Dose Response ; Drug Development ; Human ; Metabolism ; Molecular Library ; Pharmacology ; Preclinical Study ; Synthesis ; Amp-activated Protein Kinases ; Computer-aided Design ; Dose-response Relationship, Drug ; Drug Discovery ; Drug Evaluation, Preclinical ; Enzyme Activators ; Humans ; Molecular Docking Simulation ; Molecular Structure ; Small Molecule Libraries ; Structure-activity Relationship

Abstract: AMPK is a promising target for various chronic illnesses such as diabetes and Alzheimer's disease (AD). We sought to develop a novel small molecule that directly activates AMPK, with the potential to fundamentally modulate the pathogenic mechanisms of the metabolic disorders. To identify a potent novel pharmacophore in an unbiased way, we performed structure-based virtual screening on a commercially available chemical library, and evaluated the actual AMPK activity of 118 compounds selected from 100,000 compounds based on docking scores. Additional iterative molecular docking studies and experimental evaluation of AMPK activity led us to select a hit compound, B1, with a chromone backbone. Using the hit compound and other compounds structurally similar to the hit compound, we identified the chalcone structure as a new scaffold with more efficient interactions with key residues required for AMPK activation. From the newly designed and synthesized chalcone derivatives, we discovered compound 6 as a candidate compound. Compound 6 showed the most efficient interactions with the key residues of AMPK at in silico study and demonstrated significant activation of AMPK in both in vitro and in cellular assays.

Full Text: https://www.sciencedirect.com/science/article/pii/S0223523425000832

DOI: 10.1016/j.ejmech.2025.117318

Appears in Collections:: 1. College of Medicine (의과대학) > Research Institute (부설연구소) > 1. Journal Papers
1. College of Medicine (의과대학) > Dept. of Psychiatry (정신과학교실) > 1. Journal Papers

Yonsei Authors: Kim, Eosu(김어수) https://orcid.org/0000-0001-9472-9465
Kim, Hyun Jeong(김현정)

URI: https://ir.ymlib.yonsei.ac.kr/handle/22282913/208663

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