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Four mononuclear platinum(II) complexes: synthesis, DNA/BSA binding, DNA cleavage and cytotoxicity
被引:0
|作者:
Qingming Wang
Lei Yang
Jiahui Wu
Hua Wang
Jialiang Song
Xinhui Tang
机构:
[1] Yancheng Teachers’ University,School of Pharmacy, Jiangsu Provincial Key Laboratory of Coastal Wetland Bioresources and Environmental Protection
[2] Nantong University,Institute of Nautical Medicine
来源:
关键词:
Platinum(II) complexes;
DNA binding;
Bovine serum albumin (BSA) binding;
Binding modes;
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摘要:
Four new platinum(II) complexes: PtIIL1·H2O (C1, H2L1 = C20H16N2O2), PtIIL2Cl2 (C2, L2 = C22H16N2O2), PtIIL3Cl2·H2O (C3, L3 = C20H16N2), PtIIL4Cl2·0.4H2O (C4, L4 = C18H14N4) have been synthesized and characterized by using various physico-chemical techniques. The binding interaction of the four platinum(II) complexes C1–C4 with calf thymus (CT)-DNA has been investigated by UV–Vis and fluorescence emission spectrometry. The apparent binding constant (Kapp) values follow the order: C3 > C1 > C2 > C4. In addition, fluorescence spectrometry of bovine serum albumin (BSA) with the four platinum(II) complexes C1–C4 showed that the quenching mechanism might be a static quenching procedure. For C1–C4, the number of binding sites was about one for BSA and the binding constants follow the order: C3 (7.08 × 105M−1) > C1 (2.82 × 105M−1) > C2 (0.85 × 105M−1) > C4 (0.15 × 105M−1). With the single condition change such as absence of an external agent, the DNA cleavage abilities of C3 exhibit remarkable changes. In addition, the cytotoxicity of C3 in vitro on tumor cells lines (MCF-7, HepG2 and HT29) were examined by MTT and showed better antitumor effects on the tested cells.
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页码:17 / 26
页数:9
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