Du Jun, Kang Yan, Zhao Yao, Zheng Wei, Zhang Yang, Lin Yu, Wang Zhaoying, Wang Yuanyuan, Luo Qun, Wu Kui, Wang Fuyi
College of Chemistry and Materials Science, Key Laboratory of Functional Molecular Solids, the Ministry of Education, Anhui Laboratory of Molecular-Based Materials, Anhui Normal University , Wuhu 241000, People's Republic of China.
Beijing National Laboratory for Molecular Sciences; CAS Key Laboratory of Analytical Chemistry for Living Biosystems; Beijing Centre for Mass Spectrometry; Institute of Chemistry, Chinese Academy of Sciences , Beijing 100190, People's Republic of China.
Inorg Chem. 2016 May 2;55(9):4595-605. doi: 10.1021/acs.inorgchem.6b00309. Epub 2016 Apr 19.
Ruthenium-based anticancer complexes are promising antitumor agents for their low system toxicity and versatile chemical structures. Epidermal growth factor receptor (EGFR) has been found to be overexpressed in a broad range of tumor cells and is regarded as a drug target in developing novel antitumor drugs. In this work, five ruthenium(II) polypyridyl complexes containing EGFR-inhibiting 4-anilinoquinazoline pharmacophores were synthesized and characterized. These complexes showed both high EGFR-inhibiting activity and strong DNA minor groove-binding activity. In vitro antiproliferation screening demonstrated that the prepared ruthenium complexes are highly cytotoxic against a series of cancer cell lines, in particular non-small-cell lung A549 and human epidermoid carcinoma A431. Fluorescence-activated cell sorting analysis and fluorescence microscopy revealed that the most active complex, K4, induced much more late-stage cell apoptosis and necrosis than gefitinib, the first EGFR-targeting antitumor drug in clinical use. These results indicate that the ruthenium(II) polypyridyl complexes bearing EGFR-inhibiting 4-anilinoquinazolines possess highly active dual-targeting anticancer activity and are promising in developing new anticancer agents.
钌基抗癌配合物因其低系统毒性和多样的化学结构而成为有前景的抗肿瘤药物。已发现表皮生长因子受体(EGFR)在多种肿瘤细胞中过度表达,并被视为开发新型抗肿瘤药物的药物靶点。在这项工作中,合成并表征了五种含有抑制EGFR的4-苯胺基喹唑啉药效基团的钌(II)多吡啶配合物。这些配合物既表现出高EGFR抑制活性,又具有强DNA小沟结合活性。体外抗增殖筛选表明,所制备的钌配合物对一系列癌细胞系具有高度细胞毒性,尤其是对非小细胞肺癌A549和人表皮样癌A431。荧光激活细胞分选分析和荧光显微镜显示,活性最高的配合物K4比临床使用的首个EGFR靶向抗肿瘤药物吉非替尼诱导更多的晚期细胞凋亡和坏死。这些结果表明,带有抑制EGFR的4-苯胺基喹唑啉的钌(II)多吡啶配合物具有高活性双靶向抗癌活性,在开发新型抗癌药物方面具有前景。
