Mutagenic Tests Confirm That New Acetylacetonate Pt(II) Complexes Induce Apoptosis in Cancer Cells Interacting with Nongenomic Biological Targets.

Metal-Based Drugs Pub Date : 2011-01-01 Epub Date: 2011-04-10 DOI:10.1155/2011/763436

Sandra Angelica De Pascali, Federica Lugoli, Antonella De Donno, Francesco Paolo Fanizzi

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Abstract

New platinum(II) complexes [PtCl(O,O'-acac)(L)] (1) and [Pt(O,O'-acac)(γ-acac)(L)] (2) (L = DMSO, a; DMS, b) containing a single chelated (O,O'-acac) (1), or one chelated and one σ-bonded (γ-acac) acetylacetonate (2) have been synthesized. The new Pt(II) complexes exhibited high in vitro cytotoxicity on cisplatin sensitive and resistant cell lines and showed negligible reactivity with nucleobases (Guo and 5'-GMP) but selective substitution of DMSO/DMS with soft biological nucleophiles, such as L-methionine. In order to assess the ability of the new complexes with respect to cisplatin to induce apoptosis by interaction with nongenomic targets, the Ames' test, a standard reverse mutation assay, was carried out on two Salmonella typhimurium strains (TA98 and TA100). Interestingly, the new complexes did not show the well-known mutagenic activity exhibited by cisplatin and are, therefore, able to activate apoptotic pathways without interacting with DNA.

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突变试验证实新型乙酰丙酮铂(II)配合物能与非基因组生物靶点相互作用，诱导癌细胞凋亡。

合成了新的铂(II)配合物[PtCl(O,O'-acac)(L)](1)和[Pt(O,O'-acac)(γ-acac)(L)](2)（L = DMSO，a；DMS，b），它们含有单一的螯合(O,O'-acac)(1)或一个螯合和一个σ键（γ-acac）乙酰丙酮(2)。这些新的铂(II)配合物对顺铂敏感和耐药细胞株具有很高的体外细胞毒性，与核碱基（Guo 和 5'-GMP）的反应性可忽略不计，但可选择性地取代 DMSO/DMS 与 L-蛋氨酸等软生物亲核物。为了评估新复合物与顺铂相比通过与非基因组靶点相互作用诱导细胞凋亡的能力，对两种鼠伤寒沙门氏菌菌株（TA98 和 TA100）进行了艾姆斯试验（一种标准的反向突变试验）。有趣的是，新复合物并没有表现出顺铂所表现出的众所周知的诱变活性，因此能够在不与 DNA 发生相互作用的情况下激活凋亡途径。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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Metal-Based Drugs

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