Synthesis, Molecular Dynamics Simulation, and In-vitro Antitumor Activity of Quinazoline-2,4,6-triamine Derivatives as Novel EGFR Tyrosine Kinase Inhibitors.

IF 1.8 4区 医学 Q3 PHARMACOLOGY & PHARMACY Iranian Journal of Pharmaceutical Research Pub Date : 2022-12-01 DOI:10.5812/ijpr-133840
Maryam Nili Ahmadabadi, Elham Rezaee, Manijeh Nematpour, Leila Karami, Shaya Mokhtari, Farzad Kobarfard, Sayyed Abbas Tabatabai
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引用次数: 1

Abstract

Background: Developing a potent and safe scaffold is challenging in anti-cancer drug discovery.

Objectives: The study focused on developing novel series of compounds based on the inhibition of epidermal growth factor receptor tyrosine kinase (EGFR-TK) as one of the most promising compounds in cancer therapy.

Methods: In this study, a novel series of quinazoline-2,4,6-triamine derivatives were designed and synthesized through intramolecular C-H activation reaction of para-nitro aniline, trichloroacetonitrile, and isocyanides employing a one-pot reaction.

Results: The in-vitro antitumor activities of the compounds which showed acceptable inhibitory effects were investigated against breast (MCF-7), lung (A-549), and colon (HT-29) cancer cell lines by employing MTT assay. All compounds had the most negligible cytotoxicity toward normal fibroblast human cell lines. Based on structural and thermodynamics analysis results, it was found that Met 769 is a key residue in interaction with all inhibitors through the formation of hydrogen bonds with high occupancies with the amine group on the quinazoline ring of inhibitors. Also, there was a good consistency between calculated ΔG binding and experimental IC50 values of compounds 10d, 10e, and erlotinib.

Conclusions: Compound 10e had an extensive range of antitumor activity on three diverse cell lines comparable with erlotinib and doxorubicin reference drugs. Also, compound 10d showed selective cytotoxicity against cancerous lung cells (A-549). On the other side, computational studies confirmed that Met 769 is a crucial residue in interaction with all inhibitors.

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新型EGFR酪氨酸激酶抑制剂喹唑啉-2,4,6-三胺衍生物的合成、分子动力学模拟及体外抗肿瘤活性研究
背景:开发一种有效的、安全的支架是抗癌药物开发的一个挑战。目的:研究基于抑制表皮生长因子受体酪氨酸激酶(EGFR-TK)的新系列化合物,作为肿瘤治疗中最有前途的化合物之一。方法:以对硝基苯胺、三氯乙腈和异氰酸酯为原料,采用一锅反应,通过分子内C-H活化反应,设计并合成了一系列新的喹唑啉-2,4,6-三胺衍生物。结果:采用MTT法研究了化合物对乳腺癌(MCF-7)、肺癌(A-549)和结肠癌(HT-29)的体外抗肿瘤活性。所有化合物对正常成纤维人类细胞系的细胞毒性都可以忽略不计。基于结构和热力学分析结果,发现Met 769是与所有抑制剂相互作用的关键残基,通过与抑制剂的喹唑啉环上的胺基形成高占位的氢键。此外,化合物10d、10e和厄洛替尼的ΔG结合计算值与实验IC50值具有良好的一致性。结论:化合物10e对三种不同细胞系具有广泛的抗肿瘤活性,与厄洛替尼和阿霉素参比药相当。此外,化合物10d对肺癌细胞(A-549)具有选择性细胞毒性。另一方面,计算研究证实Met 769是与所有抑制剂相互作用的关键残基。
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来源期刊
CiteScore
3.40
自引率
6.20%
发文量
52
审稿时长
2 months
期刊介绍: The Iranian Journal of Pharmaceutical Research (IJPR) is a peer-reviewed multi-disciplinary pharmaceutical publication, scheduled to appear quarterly and serve as a means for scientific information exchange in the international pharmaceutical forum. Specific scientific topics of interest to the journal include, but are not limited to: pharmaceutics, industrial pharmacy, pharmacognosy, toxicology, medicinal chemistry, novel analytical methods for drug characterization, computational and modeling approaches to drug design, bio-medical experience, clinical investigation, rational drug prescribing, pharmacoeconomics, biotechnology, nanotechnology, biopharmaceutics and physical pharmacy.
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