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Design, Synthesis and Molecular Docking of New Thieno[2,3‑d]Pyrimidin‐4‐One Derivatives as Dual EGFR and FGFR Inhibitors

埃罗替尼 葡萄孢霉素 成纤维细胞生长因子受体 表皮生长因子受体抑制剂 化学 对接(动物) 体外 变构调节 药理学 癌症研究 表皮生长因子受体 生物化学 受体 生物 成纤维细胞生长因子 蛋白激酶C 医学 护理部
作者
Sara Sultan,Samar S. Tawfik,Khalid B. Selim,Magda N.A. Nasr
出处
期刊:Drug Development Research [Wiley]
卷期号:86 (1)
标识
DOI:10.1002/ddr.70061
摘要

ABSTRACT Novel thienopyrimidinone hybrids 5–25 were developed and synthesized as potential inhibitors of human EGFR and FGFR. The in vitro antiproliferative action of all compounds, towards the human breast tumor cells MDA‐MB‐231 and MCF‐7, was evaluated with doxorubicin serving as a reference (IC 50 = 6.72 µM). Compound 23 demonstrated the highest anti‐breast cancer efficacy against both cellular lines having IC 50 ranging from 2.95 to 3.80 µM. The enzyme inhibition of human EGFR and FGFR by the most active candidates 18 , 21 and 23–25 was further evaluated. Compounds 21 and 25 were the best EGFR inhibitors having IC 50 values of 0.077 and 0.059 µM, respectively, in comparison to Erlotinib (IC 50 = 0.04 µM). In comparison with Staurosporine (IC 50 = 0.024 µM), compounds 24 and 25 were the most active FGFR inhibitors having IC 50 values of 0.055 and 0.029 µM, respectively. The study of molecular docking was carried out among the most active EGFR inhibitors 21 and 25 and the most active FGFR inhibitors 24 and 25 to examine the relation between the binding pattern of these compounds with EGFR and FGFR catalytic active sites and their biological activity, whereas the computational results were aligned with the biological results. Finally, compound 25 , which was found to be the best dual inhibitor against EGFR and FGFR, was tested for inducing apoptosis and affecting cellular arrest within G2/M phase as well as it was screened to measure its safety towards normal breast cells MCF10a with IC 50 value of 47.16 µM in contrast to the reference Staurosporine (IC 50 = 18.86 µM). Accordingly, compound 25 could be considered as a potential breast cancer therapy.

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