两组具有“开环或闭环”胡椒环的吡啶 - 三唑铜配合物及其抗肿瘤活性。

Two groups of copper pyridine-triazole complexes with "open or close" pepper rings and their antitumor activities.

作者信息

Hong ZhaoGuo, Zheng Chu, Luo Bi, You Xin, Bian HeDong, Liang Hong, Chen ZhenFeng, Huang FuPing

机构信息

State Key State Key Laboratory for Chemistry and Molecular Engineering of Medicinal Resources, School of Chemistry & Pharmacy, Guangxi Normal University Guilin 541004 PR China

School of Chemistry and Chemical Engineering, Guangxi University for Nationalities, Key Laboratory of Chemistry and Engineering of Forest Products Nanning 530008 PR China.

出版信息

RSC Adv. 2020 Feb 11;10(11):6297-6305. doi: 10.1039/c9ra10677d. eCollection 2020 Feb 7.

DOI:10.1039/c9ra10677d

PMID:35496028

原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC9049676/

Abstract

Based on 1,2-dimethoxyphenyl (veratrole, open) and 1,2-methylenedioxyphenyl (pepper ring, close)-derived pyridine-triazole analogues, two groups of copper(ii) complexes, namely, Group I(C1-C3) and Group II(C4-C6) were synthesized and fully characterized. All ligands and complexes were tested by MTT assays on seven tumour cell lines (T24, Hep-G2, Sk-Ov-3, MGC-803, HeLa, A549 and NCI-H460) and one normal liver cell line (HL-7702). Surprisingly, the pepper-ring-derived complexes (C4-C6) showed significantly enhanced cytotoxicity compared with the 1,2-bimethoxyphenyl ring-derived complexes (C1-C3) and the standard anticancer drug cisplatin. Cellular uptake assays indicated that the Cu accumulation was consistent with cytotoxicity. In addition, flow cytometry and western blot analysis showed that the apoptosis of the leading complex C4 may be induced by the Bcl-2 family-mediated proteins through the mitochondrial dysfunction pathway. Furthermore, UV-vis and fluorescence spectroscopy assays revealed that C4 has stronger insertion-binding interactions with CT-DNA than C1 and the fluorescence of C1 and C4 with BSA is mainly quenched by static quenching.

摘要

基于1,2 - 二甲氧基苯基（藜芦醚，开环）和1,2 - 亚甲基二氧基苯基（胡椒环，闭环）衍生的吡啶 - 三唑类似物，合成了两组铜（II）配合物，即第一组（C1 - C3）和第二组（C4 - C6），并对其进行了全面表征。所有配体和配合物均通过MTT法在七种肿瘤细胞系（T24、Hep - G2、Sk - Ov - 3、MGC - 803、HeLa、A549和NCI - H460）和一种正常肝细胞系（HL - 7702）上进行了测试。令人惊讶的是，与1,2 - 二甲氧基苯基环衍生的配合物（C1 - C3）和标准抗癌药物顺铂相比，胡椒环衍生的配合物（C4 - C6）显示出显著增强的细胞毒性。细胞摄取实验表明，铜的积累与细胞毒性一致。此外，流式细胞术和蛋白质印迹分析表明，主要配合物C4的凋亡可能是由Bcl - 2家族介导的蛋白质通过线粒体功能障碍途径诱导的。此外，紫外 - 可见光谱和荧光光谱分析表明，C4与CT - DNA的插入结合相互作用比C1更强，并且C1和C4与BSA的荧光主要通过静态猝灭被猝灭。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/bae7/9049676/17059de3b685/c9ra10677d-f1.jpg

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两组具有“开环或闭环”胡椒环的吡啶 - 三唑铜配合物及其抗肿瘤活性。

Two groups of copper pyridine-triazole complexes with "open or close" pepper rings and their antitumor activities.

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