Targeting VEGFR-2 in breast cancer: synthesis and in silico and in vitro characterization of quinoxaline-based inhibitors†

IF 3.9 3区化学 Q2 CHEMISTRY, MULTIDISCIPLINARY

RSC Advances Pub Date : 2025-04-22 DOI:10.1039/D5RA00526D

Ibrahim H. Eissa, Alaa Elwan, Mustafa A. Al-Qadhi, Dalal Z. Husein, Fatma G. Amin, Aisha A. Alsfouk, Eslam B. Elkaeed, Hazem Elkady and Ahmed M. Metwaly

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引用次数: 0

Abstract

A novel series of quinoxaline derivatives was designed and synthesized to target VEGFR-2, a receptor critical in cancer progression, with a focus on favorable pharmacophoric features. Among these derivatives, compound 11d emerged as a promising candidate, exhibiting potent cytotoxicity against MDA-MB-231 and MCF-7 cancer cell lines, with IC₅₀ values of 21.68 μM and 35.81 μM, respectively, while displaying significantly reduced toxicity in normal cell lines WI-38 and WISH (IC₅₀ values of 82.46 μM and 75.27 μM). Compared to standard treatments doxorubicin and sorafenib, compound 11d demonstrated a favorable therapeutic window. Inhibition assays showed that 11d inhibits VEGFR-2 with an IC₅₀ of 62.26 nM ± 2.77, comparable to sorafenib. Mechanistically, treatment with 11d upregulated pro-apoptotic markers BAX, caspase-8, and caspase-9, while downregulating the anti-apoptotic marker Bcl-2, resulting in a significant BAX/Bcl-2 ratio increase (16.11). A wound healing assay confirmed 11d's anti-migratory effects, limiting wound closure in MDA-MB-231 cells to 27.51% compared to untreated cells. Additionally, flow cytometry revealed that 11d induced both early (46.43%) and late apoptosis (31.49%) in MDA-MB-231 cells, alongside G1 phase cell cycle arrest, reducing S and G2/M phase progression. Molecular docking and dynamics simulations over 200 ns demonstrated stable binding of compound 11d to VEGFR-2, with docking scores superior and comparable to sorafenib. Density Functional Theory (DFT) calculations underscored 11d's stability and reactivity, while in silico ADMET analysis predicted a favorable safety profile over sorafenib, particularly with respect to carcinogenic and chronic toxicity risks. These findings indicate that quinoxaline derivative 11d holds potential as a selective and effective VEGFR-2 inhibitor with promising antitumor and anti-metastatic properties, warranting further investigation.

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靶向乳腺癌血管内皮生长因子受体-2：基于喹喔啉的抑制剂的合成、硅学和体外表征†。

设计并合成了一系列新的喹诺啉衍生物，以VEGFR-2为靶点，VEGFR-2是癌症进展的关键受体，具有良好的药效特性。其中，化合物11d对MDA-MB-231和MCF-7癌细胞表现出较强的细胞毒性，IC50值分别为21.68 μM和35.81 μM，而对正常细胞系WI-38和WISH的毒性显著降低（IC50值分别为82.46 μM和75.27 μM）。与标准治疗阿霉素和索拉非尼相比，化合物11d显示出良好的治疗窗口。抑制实验显示，11d抑制VEGFR-2的IC50为62.26 nM±2.77，与索拉非尼相当。机制上，11d处理上调促凋亡标志物BAX、caspase-8和caspase-9，下调抗凋亡标志物Bcl-2，导致BAX/Bcl-2比值显著升高（16.11）。伤口愈合实验证实了11d的抗迁移作用，与未处理的细胞相比，MDA-MB-231细胞的伤口愈合限制在27.51%。此外，流式细胞术显示11d诱导MDA-MB-231细胞早期（46.43%）和晚期（31.49%）凋亡，同时G1期细胞周期阻滞，减少S期和G2/M期进展。超过200 ns的分子对接和动力学模拟表明，化合物11d与VEGFR-2的结合稳定，对接评分优于索拉非尼。密度泛函理论（DFT）计算强调了11d的稳定性和反应性，而计算机ADMET分析预测了sorafenib的良好安全性，特别是在致癌和慢性毒性风险方面。这些发现表明，喹诺啉衍生物11d作为一种选择性和有效的VEGFR-2抑制剂具有抗肿瘤和抗转移特性，值得进一步研究。

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来源期刊

RSC Advances chemical sciences-

CiteScore

7.50

自引率

2.60%

发文量

3116

审稿时长

1.6 months

期刊介绍： An international, peer-reviewed journal covering all of the chemical sciences, including multidisciplinary and emerging areas. RSC Advances is a gold open access journal allowing researchers free access to research articles, and offering an affordable open access publishing option for authors around the world.