通过抑制 c-MET 和 VEGFR-2 发现作为细胞凋亡诱导剂的新型 1,3-二苯基脲附加芳基吡啶衍生物:设计、合成、体内和硅学研究

IF 3.597 Q2 Pharmacology, Toxicology and Pharmaceutics
MedChemComm Pub Date : 2024-06-12 DOI:10.1039/D4MD00280F
Heba A. Elsebaie, Mohamed S. Nafie, Haytham O. Tawfik, Amany Belal, Mohammed M. Ghoneim, Ahmad J. Obaidullah, Salwa Shaaban, Abdelmoneim A. Ayed, Mohamed El-Naggar, Ahmed B. M. Mehany and Moataz A. Shaldam
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引用次数: 0

摘要

VEGFR-2 和 c-MET 作为治疗不同恶性肿瘤的潜在受体,引起了人们的兴趣。利用芳基吡啶衍生物与 1,3-二苯基脲的连接,开发并合成了一些有前景的 VEGFR-2 和 c-MET 双重抑制剂。在分子靶标方面,化合物 2d、2f、2j、2k 和 2n 对 c-MET 的有效 IC50 值分别为 65、24、150、170 和 18 nM。此外,它们对 VEGFR-2 的有效 IC50 值分别为 310、35、290、320 和 24 nM。在细胞毒性方面,化合物 2d、2f、2j、2k 和 2n 对 MCF-7 具有强效细胞毒性,IC50 值在 0.76-21.5 μM 之间;与卡博赞替尼(对 MCF-7 的 IC50 = 1.06 μM 和对 PC-3 的 IC50 = 2.01 μM)相比,它们对 PC-3 的 IC50 值在 1.85-3.42 μM 之间,显示出良好的细胞毒性活性。在细胞死亡方面,化合物 2n 可使 MCF-7 细胞死亡 87.34 倍;诱导 33.19% 的细胞凋亡(晚期凋亡为 8.04%,早期凋亡为 25.15%),使细胞在 G2/M 期停止生长,影响细胞凋亡相关基因 P53、Bax、caspases 3 和 9 以及抗凋亡基因 Bcl-2 的表达。体内研究表明,化合物 2n 具有抗癌活性,能减少肿瘤的体积和质量,肿瘤抑制率达到 56.1%,并能改善血液学指标。因此,化合物 2n 可进一步开发为针对乳腺癌的选择性靶向化疗药物。
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 new 1,3-diphenylurea appended aryl pyridine derivatives as apoptosis inducers through c-MET and VEGFR-2 inhibition: design, synthesis, in vivo and in silico studies†

Discovery of new 1,3-diphenylurea appended aryl pyridine derivatives as apoptosis inducers through c-MET and VEGFR-2 inhibition: design, synthesis, in vivo and in silico studies†

Discovery of new 1,3-diphenylurea appended aryl pyridine derivatives as apoptosis inducers through c-MET and VEGFR-2 inhibition: design, synthesis, in vivo and in silico studies†

Interest has been generated in VEGFR-2 and c-MET as potential receptors for the treatment of different malignancies. Using aryl pyridine derivatives with 1,3-diphenylurea attached, a number of promising dual VEGFR-2 and c-MET inhibitors were developed and synthesized. Regarding the molecular target, compounds 2d, 2f, 2j, 2k, and 2n had potent IC50 values of 65, 24, 150, 170, and 18 nM against c-MET, respectively. Additionally, they had potent IC50 values of 310, 35, 290, 320, and 24 nM against VEGFR-2, respectively. Regarding cytotoxicity, compounds 2d, 2f, 2j, 2k and 2n exhibited potent cytotoxicity against MCF-7 with IC50 values in the range 0.76–21.5 μM, and they showed promising cytotoxic activity against PC-3 with IC50 values in the range 1.85–3.42 μM compared to cabozantinib (IC50 = 1.06 μM against MCF-7 and 2.01 μM against PC-3). Regarding cell death, compound 2n caused cell death in MCF-7 cells by 87.34-fold; it induced total apoptosis by 33.19% (8.04% for late apoptosis, 25.15% for early apoptosis), stopping their growth in the G2/M phase, affecting the expression of apoptosis-related genes P53, Bax, caspases 3 and 9 and the anti-apoptotic gene, Bcl-2. In vivo study illustrated the anticancer activity of compound 2n by reduction of tumor mass and volume, and the tumor inhibition ratio reached 56.1% with an improvement of hematological parameters. Accordingly, compound 2n can be further developed as a selective target-oriented chemotherapeutic against breast cancer.

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来源期刊
MedChemComm
MedChemComm BIOCHEMISTRY & MOLECULAR BIOLOGY-CHEMISTRY, MEDICINAL
CiteScore
4.70
自引率
0.00%
发文量
0
审稿时长
2.2 months
期刊介绍: Research and review articles in medicinal chemistry and related drug discovery science; the official journal of the European Federation for Medicinal Chemistry. In 2020, MedChemComm will change its name to RSC Medicinal Chemistry. Issue 12, 2019 will be the last issue as MedChemComm.
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