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Crystal structure of Δ-Ru(bpy)_2dppz^(2+) bound to mismatched DNA reveals side-by-side metalloinsertion and intercalation

机译:与错配的DNA结合的Δ-Ru(bpy)_2dppz ^(2+)的晶体结构揭示了并排的金属插入和嵌入

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摘要

DNA mismatches represent a novel target in the development of diagnostics and therapeutics for cancer, because deficiencies in DNA mismatch repair are implicated in cancers, and cells that are repair-deficient show a high frequency of mismatches. Metal complexes with bulky intercalating ligands serve as probes for DNA mismatches. Here, we report the high-resolution (0.92 Å) crystal structure of the ruthenium ‘light switch’ complex Δ-[Ru(bpy)_(2)dppz]^(2+) (bpy = 2,2′-bipyridine and dppz = dipyridophenazine), which is known to show luminescence on binding to duplex DNA, bound to both mismatched and well-matched sites in the oligonucleotide 5′-(dCGGAAATTACCG)_(2)-3′ (underline denotes AA mismatches). Two crystallographically independent views reveal that the complex binds mismatches through metalloinsertion, ejecting both mispaired adenosines. Additional ruthenium complexes are intercalated at well-matched sites, creating an array of complexes in the minor groove stabilized by stacking interactions between bpy ligands and extruded adenosines. This structure attests to the generality of metalloinsertion and metallointercalation as DNA binding modes.
机译:DNA错配代表癌症诊断和治疗方法的发展中的新目标,因为DNA错配修复的缺陷与癌症有关,并且修复缺陷的细胞显示出很高的错配频率。具有庞大的嵌入配体的金属络合物可作为DNA错配的探针。在这里,我们报告了钌“光开关”络合物Δ-[Ru(bpy)_(2)dppz] ^(2 +)(bpy = 2,2'-联吡啶和dppz =二吡咯并吩嗪),已知与双链DNA结合时会发光,并与寡核苷酸5'-(dCGGAAATTACCG)_(2)-3'中错配和高度匹配的位点结合(下划线表示AA不匹配)。两种晶体学上独立的观点揭示,该配合物通过金属插入结合错配,同时弹出两个错配的腺苷。额外的钌络合物插入匹配良好的位点,从而在小沟中形成一系列络合物,这些络合物通过bpy配体与挤出的腺苷之间的堆积相互作用而稳定。这种结构证明了金属插入和金属插入作为DNA结合模式的普遍性。

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