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首页> 外文期刊>Dalton transactions: An international journal of inorganic chemistry >Synthesis and cytotoxicity of dinuclear complexes containing ruthenium(II) bipyridyl units linked by a bis(pyridylimine) ligand
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Synthesis and cytotoxicity of dinuclear complexes containing ruthenium(II) bipyridyl units linked by a bis(pyridylimine) ligand

机译:含钌(II)联吡啶单元的双核配合物的合成及细胞毒性

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Enantiopure dinuclear ruthenium polypyridyl complexes of the form [Ru-2(LL)(4)L-1](PF6)(4) (LL = 2,2'-bipyridine (bpy) or 1,10-phenanthroline (phen); L-1 = C25H20N4 a bis(pyridylimine) ligand containing a diphenylmethane spacer) have been synthesized using the chiral building blocks cis-[Ru(bpy)(2)(py)(2)](2+) and cis-[Ru(phen)(2)(py)(2)](2+). These dinuclear ruthenium complexes have been characterised using NMR, mass spectrometry, UV-visible absorbance, circular dichroism and linear dichroism. The compounds exhibit good photo and thermal stability. The extinction coefficient for the bpy complex at 478 nm is epsilon(478) = 15 700 mol(-1) cm(-1) dm(3) and for the phen complex is epsilon(478) = 24900 mol(-1) cm(-1) dm(3). Both complexes have their longest wavelength (metal to ligand charge transfer) transition predominantly x/y (short axis)-polarised while the transitions at shorter wavelength are a mixture of x/y and z-polarisations, similar to both the copper helicate and iron triple helicate studied previously. Cytotoxicity studies reveal that the compounds are dramatically less active against cancer cell lines than the recently reported supramolecular cylinders prepared from the same bis(pyridylimine) ligand.
机译:[Ru-2(LL)(4)L-1](PF6)(4)形式的对映体双核钌多吡啶基配合物(LL = 2,2'-联吡啶(bpy)或1,10-菲咯啉(phen); L-1 = C25H20N4已使用手性构件cis- [Ru(bpy)(2)(py)(2)](2+)和cis- [Ru合成了含二苯基甲烷间隔基的双(吡啶基嘧啶)配体) (phen)(2)(py)(2)](2+)。这些双核钌配合物已使用NMR,质谱,紫外可见吸收率,圆二色性和线性二色性进行了表征。这些化合物表现出良好的光稳定性和热稳定性。 bpy络合物在478 nm处的消光系数为epsilon(478)= 15700 mol(-1)cm(-1)dm(3),而phen络合物的消光系数为epsilon(478)= 24900 mol(-1)cm (-1)dm(3)。两种络合物都具有最长的波长(金属到配体电荷转移)过渡,主要是x / y(短轴)极化,而在较短波长下的过渡是x / y和z极化的混合物,类似于螺旋铜和铁以前研究过的三重螺旋。细胞毒性研究表明,该化合物对癌细胞系的活性远低于最近报道的由相同双(吡啶并嘧啶)配体制备的超分子圆柱体。

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