Design, In Silico Molecular Docking, and ADMET Prediction of Amide Derivatives of Chalcone Nucleus as EGFR Inhibitors for the Treatment of Cancer.

Shital Patil, Vrushali Randive, Indrani Mahadik, Kalyani Asgaonkar
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Abstract

Background: Cancer is a devastating disease. Many studies have shown that the primary causes of the aggressive and resistant types of cancer are the overexpression of receptors and growth factors, activation of oncogenes, and the inactivation of tumour suppressor genes. One such receptor is the epidermal growth factor receptor (EGFR), which is used as a drug target for the treatment of cancer.

Objective: This study aimed to develop the new chemical entities of amide derivatives of chalcone as EGFR inhibitors using structure-activity relationship (SAR) studies, molecular docking, and ADMET (absorption, distribution, metabolism, excretion, and toxicity) studies.

Method: New chemical entities (NCE) were designed based on literature findings. The Schrodinger 13.4 software was used for the molecular docking study. While Quickprop and Pro Tox-II online tools were used for ADME and toxicity prediction, respectively. .

Result: In this work, all compounds were subjected to an in-silico ADMET analysis. After pharmacokinetic and toxicity profile predictions, the molecules were further analysed by molecular docking. As a result of molecular docking, molecules AC9 and AC19 showed comparable docking scores compared to standard Afatinib.

Conclusion: Molecules AC9 and AC19 showed good docking scores and a promising ADMET profile. In the future, these derivatives can be further evaluated for wet lab studies and determination of their biological activity.

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Chalcone核酰胺衍生物作为EGFR抑制剂治疗癌症的设计、硅内分子对接和ADMET预测。
背景:癌症是一种毁灭性疾病。许多研究表明,癌症侵袭性和抗性类型的主要原因是受体和生长因子的过度表达、致癌基因的激活以及肿瘤抑制基因的失活。一种这样的受体是表皮生长因子受体(EGFR),其被用作治疗癌症的药物靶点。目的:本研究旨在通过结构-活性关系(SAR)研究、分子对接和ADMET(吸收、分布、代谢、排泄和毒性)研究,开发查尔酮酰胺衍生物作为EGFR抑制剂的新化学实体。方法:根据文献资料设计新的化学实体(NCE)。薛定谔13.4软件用于分子对接研究。而Quickprop和Pro Tox II在线工具分别用于ADME和毒性预测。结果:在这项工作中,所有化合物都进行了计算机ADMET分析。在药代动力学和毒性预测后,通过分子对接对分子进行进一步分析。作为分子对接的结果,与标准阿法替尼相比,分子AC9和AC19显示出可比较的对接得分。结论:分子AC9和AC19显示出良好的对接得分和有前景的ADMET图谱。未来,这些衍生物可以进一步评估,用于湿实验室研究和测定其生物活性。
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