Molecular modeling and cytotoxic activity studies of oxirane-2-carboxylate derivatives.

IF 2.7 3区 生物学 Q3 BIOCHEMISTRY & MOLECULAR BIOLOGY Journal of Biomolecular Structure & Dynamics Pub Date : 2024-11-15 DOI:10.1080/07391102.2024.2428826
Muhammed Tilahun Muhammed, Mustafa Er, Senem Akkoc
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Abstract

In this study, five 3-aryloxirane-2-carboxylate derivatives were prepared, and the antiproliferative activities of molecules were screened in lung and colon cancer cell lines. The results showed that molecules had antiproliferative activity on cancerous cells with IC50 values under 100 µM. Furthermore, all of the molecules were found to have a much higher cytotoxic effect than cisplatin in colon cancer cells. The interactions of the relatively active compounds to the crucial enzyme in cancer cell proliferation, cyclin-dependent kinase 1 (CDK1), were investigated using molecular docking. The stability of the resulting CDK1-compound complexes procured from the docking was also assessed through molecular dynamics (MD) simulations. Then, the binding affinity of compounds 2-3a and 2-3c to the target enzyme was computed by MMPBSA. The molecular docking study demonstrated that the two most active compounds could bind to the enzyme. The binding potential of 2-3a is anticipated to be higher as it had one more conventional hydrogen bond and a slightly lower binding energy than compound 2-3c. The MD simulation study exhibited that the two compounds formed a stable complex with the enzyme. On the other hand, the MMPBSA energy computation implicated a slightly higher binding affinity for compound 2-3c toward the enzyme. Furthermore, electrical and frontier molecular orbital analysis of all of the tested compounds was conducted by density functional theory (DFT) studies. Compound 2-3a is anticipated to be the most chemically stable as it gave the highest energy gap value in the DFT analysis.

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环氧乙烷-2-羧酸酯衍生物的分子建模和细胞毒性活性研究。
本研究制备了五种 3-芳基环氧乙烷-2-甲酸酯衍生物,并在肺癌和结肠癌细胞系中对这些分子的抗增殖活性进行了筛选。结果表明,这些分子对癌细胞具有抗增殖活性,其 IC50 值低于 100 µM。此外,还发现所有分子对结肠癌细胞的细胞毒性作用都远远高于顺铂。分子对接法研究了相对活跃的化合物与癌细胞增殖的关键酶--细胞周期蛋白依赖性激酶 1(CDK1)的相互作用。此外,还通过分子动力学(MD)模拟评估了通过对接得到的 CDK1-化合物复合物的稳定性。然后,通过 MMPBSA 计算了化合物 2-3a 和 2-3c 与目标酶的结合亲和力。分子对接研究表明,两种活性最强的化合物都能与酶结合。预计 2-3a 的结合势能较高,因为它比化合物 2-3c 多一个常规氢键,结合能略低。MD 模拟研究表明,这两种化合物与酶形成了稳定的复合物。另一方面,MMPBSA 能量计算表明,化合物 2-3c 与酶的结合亲和力略高。此外,还通过密度泛函理论(DFT)研究对所有测试化合物进行了电性和前沿分子轨道分析。预计化合物 2-3a 的化学性质最为稳定,因为它在 DFT 分析中给出了最高的能隙值。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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来源期刊
Journal of Biomolecular Structure & Dynamics
Journal of Biomolecular Structure & Dynamics 生物-生化与分子生物学
CiteScore
8.90
自引率
9.10%
发文量
597
审稿时长
2 months
期刊介绍: The Journal of Biomolecular Structure and Dynamics welcomes manuscripts on biological structure, dynamics, interactions and expression. The Journal is one of the leading publications in high end computational science, atomic structural biology, bioinformatics, virtual drug design, genomics and biological networks.
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