首页> 外文期刊>European Journal of Medicinal Chemistry: Chimie Therapeutique >Biological activity of neutral and cationic iridium(III) complexes with κp and κp,κS coordinated Ph2PCH2S(O) xPh (x = 0-2) ligands
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Biological activity of neutral and cationic iridium(III) complexes with κp and κp,κS coordinated Ph2PCH2S(O) xPh (x = 0-2) ligands

机译:具有κp和κp,κS配位的Ph2PCH2S(O)xPh(x = 0-2)配体的中性和阳离子铱(III)配合物的生物活性

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Neutral iridium(III) complexes of the type [Ir(η5-C 5Me5)Cl2{Ph2PCH2S(O) xPh-κP}] (1-3) with diphenylphosphino-functionalized methyl phenyl sulfides, sulfoxides, and sulfones Ph2PCH2S(O) xPh (x = 0, L1; 1, L2; 2, L3) and the cationic complex [Ir(η5-C5Me5)Cl{Ph2PCH 2SPh-κP,κS}][PF6] (4) were synthesized and fully characterized analytically and spectroscopically. Furthermore, the structure of 2 was determined by X-ray diffraction analysis. The biological potential of the neutral and cationic iridium(III) complexes was tested in vitro against the cell lines 8505C, A253, MCF-7, SW480 and 518A2. Complex [Ir(η5-C5Me5)Cl2{Ph 2PCH2S(O)Ph-κP}] (2), with ligand L2 κP coordinated containing a pendent sulfinyl group, is the most active one (IC 50 values of about 3 μM), thus, with activities comparable to cisplatin. Complex 2 proved to have an even a higher antiproliferative activity than cisplatin against 8505C and SW480 cell lines, used as a model system of highly anaplastic cancers with low sensitivity to conventional chemotherapeutics such as cisplatin. Additional experiments demonstrated that apoptosis and autophagic cell death contribute to the drug's tumoricidal action.
机译:[Ir(η5-C5Me5)Cl2 {Ph2PCH2S(O)xPh-κP}](1-3)类型的中性铱(III)配合物与二苯基膦基官能化的甲基苯基硫化物,亚砜和砜Ph2PCH2S(O)xPh (x = 0,L1; 1,L2; 2,L3)和阳离子络合物[Ir(η5-C5Me5)Cl {Ph2PCH2SPh-κP,κS}] [PF6](4)合成并通过分析和光谱学充分表征。此外,通过X射线衍射分析确定2的结构。在体外针对细胞系8505C,A253,MCF-7,SW480和518A2测试了中性和阳离子铱(III)配合物的生物潜力。络合物[Ir(η5-C5Me5)Cl2 {Ph 2PCH2S(O)Ph-κP}](2)是最活泼的化合物(IC 50值为约3μM),配位体L2κP配体包含一个亚磺酰基。因此,具有与顺铂相当的活性。事实证明,配合物2对于8505C和SW480细胞系具有比顺铂更高的抗增殖活性,被用作高度变性癌症的模型系统,对常规化学疗法(如顺铂)的敏感性较低。其他实验表明,细胞凋亡和自噬细胞死亡有助于药物的杀肿瘤作用。

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