Discovery of 5-Hydroxy-1,4-naphthoquinone (Juglone) Derivatives as Dual Effective Agents Targeting Platelet-Cancer Interplay through Protein Disulfide Isomerase Inhibition.
Yu-Pu JuangJu-Ying TsaiWan-Lan GuHui-Ching HsuChao-Lung LinChin-Chung WuPi-Hui LiangPublished in: Journal of medicinal chemistry (2024)
In this study, a series of 2- and/or 3-substituted juglone derivatives were designed and synthesized. Among them, 9 , 18 , 22 , 30 , and 31 showed stronger inhibition activity against cell surface PDI or recombinant PDI and higher inhibitory effects on U46619- and/or collagen-induced platelet aggregation than juglone. The glycosylated derivatives 18 and 22 showed improved selectivity for inhibiting the proliferation of multiple myeloma RPMI 8226 cells, and the IC 50 values reached 61 and 48 nM, respectively, in a 72 h cell viability test. In addition, 18 and 22 were able to prevent tumor cell-induced platelet aggregation and platelet-enhanced tumor cell proliferation. The molecular docking showed the amino acid residues Gln243, Phe440, and Leu443 are important for the compound-protein interaction. Our results reveal the potential of juglone derivatives to serve as novel antiplatelet and anticancer dual agents, which are available to interrupt platelet-cancer interplay through covalent binding to PDI catalytic active site.
Keyphrases
- papillary thyroid
- molecular docking
- amino acid
- cell proliferation
- cell surface
- multiple myeloma
- high glucose
- signaling pathway
- diabetic rats
- single cell
- induced apoptosis
- molecular dynamics simulations
- stem cells
- drug induced
- protein protein
- photodynamic therapy
- high throughput
- mesenchymal stem cells
- cell cycle
- endothelial cells
- oxidative stress
- cell therapy
- structure activity relationship
- pi k akt
- cell cycle arrest
- endoplasmic reticulum stress
- stress induced
- human health