Faculty of Chemistry, Islamic Azad University, North Tehran Branch, Tehran, Iran.
Research Center for Traditional Medicine and History of Medicine, Department of Persian Medicine, School of Medicine, Shiraz University of Medical Sciences, Shiraz, Iran.
Sci Rep. 2024 Jan 17;14(1):1540. doi: 10.1038/s41598-024-52022-6.
A series of new analogs of 3,5-dihydroxybenzoyl-hydrazineylidene conjugated to different methoxyphenyl triazole (11a-n) synthesized using click reaction. The structures of all synthesized compounds were characterized by FTIR, H, C-NMR spectroscopy, and CHO analysis. The tyrosinase inhibitory potential of the synthesized compounds was studied. The newly synthesized scaffolds were found to illustrate the variable degree of the inhibitory profile, and the most potent analog of this series was that one bearing 4-methoxyphenyl moiety, and exhibited an IC value of 55.39 ± 4.93 µM. The kinetic study of the most potent derivative reveals a competitive mode of inhibition. Next, molecular docking studies were performed to understand the potent inhibitor's binding mode within the enzyme's binding site. Molecular dynamics simulations were accomplished to further investigate the orientation and binding interaction over time and the stability of the 11m-tyrosinase complex.
使用点击反应合成了一系列新的 3,5-二羟基苯甲酰基腙与不同甲氧基苯基三唑(11a-n)的类似物。所有合成化合物的结构均通过 FTIR、H、C-NMR 光谱和 CHO 分析进行了表征。研究了合成化合物的酪氨酸酶抑制潜力。新合成的支架表明具有不同程度的抑制谱,该系列中最有效的类似物是带有 4-甲氧基苯基部分的类似物,其 IC 值为 55.39±4.93µM。最有效的衍生物的动力学研究表明其抑制模式为竞争性。接下来,进行了分子对接研究以了解有效抑制剂在酶结合位点内的结合模式。进行了分子动力学模拟,以进一步研究在时间和 11m-酪氨酸酶复合物的稳定性上的取向和结合相互作用。
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