发现取代的 2-oxoquinolinylthiazolidin-4-one 类似物作为肺癌治疗中潜在的表皮生长因子受体 K 抑制剂。

IF 1.7 Q3 PHARMACOLOGY & PHARMACY
Drug Research Pub Date : 2024-06-01 Epub Date: 2024-06-03 DOI:10.1055/a-2305-2789
Soniya Naik, Vasu Soumya, Shivlingrao N Mamledesai, M Manickavasagam, Prafulla Choudhari, Sanket Rathod
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引用次数: 0

摘要

目的:癌症是全球第二大死因,2018 年估计有 960 万人死于癌症。在全球范围内,大约每 6 人中就有 1 人死于癌症,而现有的化疗药物具有毒性高、副作用大的特点,因此需要合成治疗癌症的新型药物:目前的研究工作涉及一系列 3-(3-乙酰基-2-氧代喹啉-1-(2H)-基-2-(取代苯基)噻唑烷-4-酮(Va-j)衍生物的合成及其体外抗癌活性评估。所有合成的化合物都通过红外和核磁共振数据得到了令人满意的表征。研究人员进一步评估了这些化合物对 A-549(肺癌)细胞系的体外抗癌活性。体外抗癌活性基于 3-(4,5-二甲基噻唑-2-基)-2,5-二苯基溴化四氮唑(MTT)测定法:合成的化合物对 A-549 细胞株具有令人满意的抗癌特性。化合物(VH):在所测试的衍生物中对 A-549 细胞株显示出最高的效力,IC50 值分别为 100 µg/ml,而且比作为标准药物的伊马替尼(150 µg/ml)更有效。使用 AutoDock Vina/PyRx 软件对标题化合物(Va-j)进行了分子对接研究。合成的化合物与表皮生长因子受体激酶酪氨酸激酶结构域(PDB 1m17)活性口袋中的一个或多个氨基酸残基形成了保留良好的氢键:结论:在所有合成的类似物中,化合物(Vh)的结合亲和力高于其他合成的衍生物,分子动力学模拟研究探讨了对接复合物系统的稳定性。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Discovery of Substituted 2-oxoquinolinylthiazolidin-4-one Analogues as Potential EGFRK Inhibitors in Lung Cancer Treatment.

Purpose: Cancer is the second leading cause of death globally and is responsible for an estimated 9.6 million deaths in 2018. Globally, about 1 in 6 deaths is due to cancer and the chemotherapeutic drugs available have high toxicity and have reported side effects hence, there is a need for the synthesis of novel drugs in the treatment of cancer.

Methods: The current research work dealt with the synthesis of a series of 3-(3-acetyl-2-oxoquinolin-1-(2H)-yl-2-(substitutedphenyl)thiazolidin-4-one (Va-j) derivatives and evaluation of their in-vitro anticancer activity. All the synthesized compounds were satisfactorily characterized by IR and NMR data. Compounds were further evaluated for their in-vitro anticancer activity against A-549 (lung cancer) cell lines. The in-vitro anticancer activity was based upon the 3-(4,5-dimethylthiazol-2-yl)-2,5-diphenyltetrazoliumbromide (MTT) assay method.

Results: The synthesized compounds exhibited satisfactory anticancer properties against the A-549 cell line. The compound (VH): showed the highest potency amongst the tested derivatives against the A-549 cell line with IC50 values of 100 µg/ml respectively and was also found to be more potent than Imatinib (150 µg/ml) which was used as a standard drug. Molecular docking studies of the titled compounds (Va-j) were carried out using AutoDock Vina/PyRx software. The synthesized compounds exhibited well-conserved hydrogen bonds with one or more amino acid residues in the active pocket of the EGFRK tyrosine kinase domain (PDB 1m17).

Conclusion: Among all the synthesized analogues, the binding affinity of the compound (Vh) was found to be higher than other synthesized derivatives and a molecular dynamics simulation study explored the stability of the docked complex system.

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来源期刊
Drug Research
Drug Research PHARMACOLOGY & PHARMACY-
CiteScore
3.50
自引率
0.00%
发文量
67
期刊介绍: Drug Research (formerly Arzneimittelforschung) is an international peer-reviewed journal with expedited processing times presenting the very latest research results related to novel and established drug molecules and the evaluation of new drug development. A key focus of the publication is translational medicine and the application of biological discoveries in the development of drugs for use in the clinical environment. Articles and experimental data from across the field of drug research address not only the issue of drug discovery, but also the mathematical and statistical methods for evaluating results from industrial investigations and clinical trials. Publishing twelve times a year, Drug Research includes original research articles as well as reviews, commentaries and short communications in the following areas: analytics applied to clinical trials chemistry and biochemistry clinical and experimental pharmacology drug interactions efficacy testing pharmacodynamics pharmacokinetics teratology toxicology.
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