纳布美酮新型异恶唑啉和吡唑啉衍生物对乳腺癌细胞株MCF-7抗肿瘤活性的分子对接研究及体外评价

Kanar Muthanna Alawad, M. Mahdi, Ayad M. R. Raauf
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引用次数: 6

摘要

设计、合成了多种新型吡唑啉、异恶唑啉和酰胺衍生物,并在体外测试了它们对乳腺癌细胞系MCF-7的细胞毒性。那布美酮是一种用作非甾体抗炎药(NSAID)的前药。在合成前,使用分子对接程序(GOLD suite v. 5.7.1)评估ER-α受体的选择性,结果与体外实验结果一致。具体来说,靶向ER- α受体的化合物1e和2e的PLP适应度值最高,分别为75.61和73.36,而他莫昔芬参考药物的PLP适应度为92.78。合成化合物的IC50值表明,化合物(1e)对MCF-7的IC50值为19µM,而他莫昔芬的IC50值为(18.02)µM。
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Molecular Docking study, and In vitro Evaluation of Antitumor Activity of Some New Isoxazoline and Pyrazoline Derivatives of Nabumetone against breast cancer cell line (MCF-7)
A variety of new pyrazolines, isoxazolines, and amide derivatives were designed, synthesized, and tested in vitro for their cytotoxic potential against the breast cancer cell line MCF-7. Nabumetone is a prodrug that is used as non-steroidal anti-inflammatory drug   (NSAID). Before synthesis, the Molecular docking program (GOLD suite v. 5.7.1) was used to evaluate the selectivity for ER-α receptor, which demonstrated good agreement with the in vitro findings. Specifically, compounds 1e and 2e that target the ER- α receptor had the greatest PLP fitness values of (75.61 and 73.36), respectively, when compared to the tamoxifen reference medication, which had a PLP fitness of (92.78). The IC50 values for the synthesized compounds revealed that compound (1e) has a high IC50 value of 19 µM against MCF-7, compared to tamoxifen, which has an IC50 value of (18.02) µM.  
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