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首页> 外文期刊>European Journal of Medicinal Chemistry: Chimie Therapeutique >Synthetic, structural and biochemical studies of polynuclear platinum(II) complexes with heterocyclic ligands.
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Synthetic, structural and biochemical studies of polynuclear platinum(II) complexes with heterocyclic ligands.

机译:具有杂环配体的多核铂(II)配合物的合成,结构和生化研究。

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摘要

"Non-classical" di- and trinuclear Pt(II) complexes with polydentate nitrogen ligands; ionic [(PtCl(2))(2)(tptz)(2)(mu-PtClNCPh)]Cl (1) [tptz =2,4,6-tris(2-pyridyl)-1,3,5-triazine], [(PtCl(2))(2)(bptz)(2)(mu-Pt)]Cl(2) (2) [bptz = 3,6-bis(2-pyridyl)-1,2,4,5-tetrazine] and neutral [(PtCl(2))(2)(tptz)(2)(mu-PtCl(2))](H(2)O)(4) (3), [(PtCl(2))(2)(mu-tppz)](CHCl(3)) (4) [tppz = 2,3,5,6-tetra(2-pyridyl)pyrazine] complexes, have been prepared and structurally characterized. The neutral tptz and tppz complexes present three and two separate PtCl(2) moieties, respectively, in a cis position, presumably acting in a bifunctional mode towards DNA; the cationic tptz and bptz complexes contain monofunctional and bifunctional bridging Pt(II) moieties, respectively, (other Pt(II) moieties in the complexes are bifunctional). All complexes were tested for their biological activity. Both tptz complexes, neutral and ionic, show a potent cytotoxic activity and reduced cell viability in a concentration-dependent manner thatwas evaluated in a panel of different cancer cell lines: human HT29 colon-rectal carcinoma, HepG2 hepatoma, MDA-MB-231 breast cancer and MG63 osteosarcoma cells; their activity was higher than cisplatin, IC50 values have been calculated for the active compounds and flow cytometric analysis for the tptz complexes performed. Therefore, these new platinum drugs warrant further investigation into their antitumor activity against different types of tumors.
机译:具有多齿氮配体的“非经典”二核和三核Pt(II)配合物;离子性[[PtCl(2))(2)(tptz)(2)(mu-PtClNCPh)] Cl(1)[tptz = 2,4,6-三(2-吡啶基)-1,3,5-三嗪],[(PtCl(2))(2)(bptz)(2)(mu-Pt)] Cl(2)(2)[bptz = 3,6-双(2-吡啶基)-1,2,4 ,5-tetrazine]和中性[[PtCl(2))(2)(tptz)(2)(mu-PtCl(2))](H(2)O)(4)(3),[(PtCl( 2))(2)(mu-tppz)](CHCl(3))(4)[tppz = 2,3,5,6-四(2-吡啶基)吡嗪]配合物已经制备并进行了结构表征。中性的tptz和tppz配合物分别在顺式位置呈现三个和两个单独的PtCl(2)部分,大概是对DNA的双功能模式。阳离子tptz和bptz配合物分别包含单功能和双功能桥接Pt(II)部分(配合物中的其他Pt(II)部分是双功能的)。测试所有复合物的生物活性。两种tptz复合物(中性和离子型)均显示出有效的细胞毒活性,并以浓度依赖性的方式降低了细胞活力,已在一系列不同的癌细胞系中进行了评估:人HT29结肠直肠癌,HepG2肝癌,MDA-MB-231乳腺癌癌症和MG63骨肉瘤细胞;它们的活性高于顺铂,已计算出活性化合物的IC50值,并进行了tptz配合物的流式细胞术分析。因此,这些新的铂类药物需要进一步研究其对不同类型肿瘤的抗肿瘤活性。

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