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Macakurzin C Derivatives as a Novel Pharmacophore for Pan-Peroxisome Proliferator-Activated Receptor Modulatoroa mark
  • Ko, Hyejin ;
  • An, Seungchan ;
  • Jang, Hongjun ;
  • Ahn, Sungjin ;
  • Park, In Guk ;
  • Hwang, Seok Young ;
  • Gong, Junpyo ;
  • Oh, Soyeon ;
  • Kwak, Soo Yeon ;
  • Choi, Won Jun ;
  • Kim, Hyoungsu ;
  • Noh, Minsoo
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Publication Year
2023-05-01
Publisher
Korean Society of Applied Pharmacology
Citation
Biomolecules and Therapeutics, Vol.31, pp.312-318
Keyword
AdiponectinHuman bone marrow mesenchymal stem cellsMacakurzin C derivativePeroxisome proliferator-activated receptorPPARα/γ dual modulator
All Science Classification Codes (ASJC)
BiochemistryMolecular MedicinePharmacologyDrug Discovery
Abstract
The natural flavonoid macakurzin C (1) exhibited adiponectin biosynthesis-inducing activity during adipogenesis in human bone marrow mesenchymal stem cells and its molecular mechanism was directly associated with a pan-peroxisome proliferator-activat-ed receptor (PPAR) modulator affecting all three PPAR subtypes α, γ, and δ. In this study, increases in adiponectin biosynthesis-inducing activity by macakurzin C derivatives (2–7) were studied. The most potent adiponectin biosynthesis-inducing compound 6, macakurzin C 3,5-dimethylether, was elucidated as a dual PPARα/γ modulator. Compound 6 may exhibit the most potent activity because of the antagonistic relationship between PPARδ and PPARγ. Docking studies revealed that the O-methylation of macakurzin C to generate compound 6 significantly disrupted PPARδ binding. Compound 6 has therapeutic potential in hypoadi-ponectinemia-related metabolic diseases.
Language
eng
URI
https://dspace.ajou.ac.kr/dev/handle/2018.oak/33407
DOI
https://doi.org/10.4062/biomolther.2022.097
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Type
Article
Funding
This study was supported by the National Research Foundation of Korea (NRF) grants funded by the Korea government (MSIT) [NRF-2019R1A2C2085749, NRF-2022M3A9B6017654, and NRF-2020R1A2C2010329].
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