Discovery of Novel Pyrimidine Based Small Molecule Inhibitors as VEGFR-2 Inhibitors: Design, Synthesis, and Anti-Cancer Studies.

Sachin A Dhawale, Santosh N Mokale, Pratap S Dabhade
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Abstract

Background: Receptor tyrosine kinases (RTKs) are potent oncoproteins in cancer that, when mutated or overexpressed, can cause uncontrolled growth of cells, angiogenesis, and metastasis, making them significant targets for cancer treatment. Vascular endothelial growth factor receptor 2 (VEGFR2), is a tyrosine kinase receptor that is produced in endothelial cells and is the most crucial regulator of angiogenic factors involved in tumor angiogenesis. So, a series of new substituted N-(4-((2-aminopyrimidin-5-yl)oxy)phenyl)-N-phenyl cyclopropane1,1-dicarboxamide derivatives as VEGFR-2 inhibitors have been designed and synthesized.

Methods: Utilizing H-NMR, C13-NMR, and mass spectroscopy, the proposed derivatives were produced and assessed. HT-29 and COLO-205 cell lines were used for the cytotoxicity tests. The effective compound was investigated further for the Vegfr-2 kinase inhibition assay, cell cycle arrest, and apoptosis. A molecular docking examination was also carried out with the Maestro-12.5v of Schrodinger.

Results: In comparison to the reference drug Cabozantinib (IC50 = 9.10 and 10.66 µM), compound SP2 revealed promising cytotoxic activity (IC50 = 4.07 and 4.98 µM) against HT-29 and COLO-205, respectively. The synthesized compound SP2 showed VEGFR-2 kinase inhibition activity with (IC50 = 6.82 µM) against the reference drug, Cabozantinib (IC50 = 0.045 µM). Moreover, compound SP2 strongly induced apoptosis by arresting the cell cycle in the G1 phase. The new compounds' potent VEGFR-2 inhibitory effect was noted with key amino acids Asp1044, and Glu883, and the hydrophobic interaction was also observed in the pocket of the VEGFR-2 active site by using a docking study.

Conclusion: The results demonstrate that at the cellular and enzyme levels, the synthetic compounds SP2 are similarly effective as cabozantinib. The cell cycle and apoptosis data demonstrate the effectiveness of the suggested compounds. Based on the findings of docking studies, cytotoxic effects, in vitro VEGFR-2 inhibition, apoptosis, and cell cycle arrest, this research has given us identical or more effective VEGFR-2 inhibitors.

发现新型嘧啶基小分子抑制剂作为 VEGFR-2 抑制剂:设计、合成和抗癌研究。
背景:受体酪氨酸激酶(RTK)是癌症中的强效癌蛋白,一旦发生突变或过度表达,就会导致细胞失控生长、血管生成和转移,从而成为癌症治疗的重要靶点。血管内皮生长因子受体 2(VEGFR2)是内皮细胞中产生的一种酪氨酸激酶受体,是参与肿瘤血管生成的血管生成因子的最重要调节因子。因此,我们设计并合成了一系列新的取代 N-(4-((2-氨基嘧啶-5-基)氧基)苯基)-N-苯基环丙烷-1,1-二甲酰胺衍生物作为 VEGFR-2 抑制剂:方法:利用 H-NMR、C13-NMR 和质谱,制备并评估了拟议的衍生物。采用 HT-29 和 COLO-205 细胞系进行细胞毒性测试。进一步研究了有效化合物的 Vegfr-2 激酶抑制实验、细胞周期停滞和细胞凋亡。此外,还使用 Schrodinger 的 Maestro-12.5v 进行了分子对接测试:与参考药物卡博替尼(IC50 = 9.10 和 10.66 µM)相比,化合物 SP2 对 HT-29 和 COLO-205 分别显示出良好的细胞毒性活性(IC50 = 4.07 和 4.98 µM)。合成的化合物 SP2 具有 VEGFR-2 激酶抑制活性(IC50 = 6.82 µM),而参考药物 Cabozantinib 的 IC50 = 0.045 µM。此外,化合物 SP2 还能使细胞周期停滞在 G1 期,从而强烈诱导细胞凋亡。新化合物对VEGFR-2的强效抑制作用与关键氨基酸Asp1044和Glu883有关,通过对接研究还在VEGFR-2活性位点的口袋中观察到了疏水相互作用:结果表明,在细胞和酶水平上,合成化合物 SP2 与卡博替尼有相似的疗效。细胞周期和细胞凋亡数据证明了建议化合物的有效性。根据对接研究、细胞毒性作用、体外 VEGFR-2 抑制、细胞凋亡和细胞周期停滞的结果,这项研究为我们提供了相同或更有效的 VEGFR-2 抑制剂。
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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