纳布美酮新型吡啶衍生物的合成、表征、分子对接、硅ADME研究及体外细胞毒性评价。

Bushra K. Jameel, Ayad M. R. Raauf, Wassan Abdul, Kareem Abbas
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摘要

合成了含有2-氨基- 3-氰基基团的萘美酮吡啶衍生物,旨在通过两种方法引入新的EGFR激酶抑制剂:一种是先合成查尔酮衍生物(1a-d),然后与丙二腈和乙酸铵反应形成(2a-d),另一种是将所有反应物一起一锅合成化合物(2a-e)。采用熔点、红外光谱对合成的化合物进行了表征,并通过1H-NMR和13C-NMR进行了验证。最终化合物(2a-e)在体外对A549(肺癌细胞系)和WRL68(人正常细胞系)的作用进行了研究。化合物(2a、2b和2e)的IC50分别为24.62、23.43和24.06 μg/ml,显著高于对照药物厄洛替尼的IC50 (25 μg/ml)。选择性指数(SI)的测定表明,所有化合物都具有较高的选择性,特别是化合物(2a)对癌细胞的选择性最高,而不是正常细胞,SI比厄洛替尼高2倍。分子对接研究显示与EGFR激酶结合良好,与MTT检测结果有良好的相关性。在硅片上的ADME研究表明,该合成系列不仅具有有趣的活性,而且具有良好的药代动力学特性。
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Synthesis, characterization, molecular docking, in silico ADME study, and in vitro cytotoxicity evaluation of new pyridine derivatives of nabumetone.
New pyridine derivatives of nabumetone containing 2-amino 3-cyano moieties were synthesized and aimed to introduce new EGFR kinase inhibitors through two methods either by synthesis of chalcone derivatives initially (1a-d) followed by reacting it with malononitrile and ammonium acetate to form (2a-d) or from a one-pot synthesis of all reactants together to synthesis compounds (2a-e). Melting point, and FT-IR spectra were used to characterize all the synthesized compounds and were confirmed by 1H-NMR, and 13C-NMR spectroscopy. The final compounds (2a-e) were investigated in vitro against A549 (lung cancer cell line) and WRL68 (human normal cell line). compounds (2a, 2b, and 2e) produced marked cytotoxic activity with IC50 (24.62, 23.43, and 24.06 μg/ml) respectively, higher than what obtained from erlotinib with IC50 (25 μg/ml) as a reference drug. Measuring the selectivity index (SI) reveals that all the compounds have high selectivity especially compound (2a) being the most selective towards cancerous cells rather than normal cells with SI two folds higher than erlotinib. The molecular docking study reveals good binding to the EGFR kinase that has a good correlation to the MTT Assay results. In silico ADME study exposes that this synthesized series not only have interesting activity but also shows promised pharmacokinetic properties.
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