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DNA microstructure influences selective binding of small molecules designed to target mixed-site DNA sequences

机译:DNA的微观结构影响旨在靶向混合位点DNA序列的小分子的选择性结合

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摘要

Specific targeting of protein–nucleic acid interactions is an area of current interest, for example, in the regulation of gene-expression. Most transcription factor proteins bind in the DNA major groove; however, we are interested in an approach using small molecules to target the minor groove to control expression by an allosteric mechanism. In an effort to broaden sequence recognition of DNA-targeted-small-molecules to include both A·T and G·C base pairs, we recently discovered that the heterocyclic diamidine, DB2277, forms a strong monomer complex with a DNA sequence containing 5΄-AAAGTTT-3΄. Competition mass spectrometry and surface plasmon resonance identified new monomer complexes, as well as unexpected binding of two DB2277 with certain sequences. Inherent microstructural differences within the experimental DNAs were identified through computational analyses to understand the molecular basis for recognition. These findings emphasize the critical nature of the DNA minor groove microstructure for sequence-specific recognition and offer new avenues to design synthetic small molecules for effective regulation of gene-expression.
机译:蛋白质-核酸相互作用的特异性靶向是当前关注的领域,例如,在基因表达的调控中。大多数转录因子蛋白都结合在DNA主沟中。但是,我们对使用小分子靶向小沟以通过变构机制控制表达的方法感兴趣。为了扩大对DNA靶向小分子的序列识别,使其既包括A·T碱基又包括G·C碱基对,我们最近发现杂环二amDB2277与包含5' -AAAGTTT-3΄。竞争质谱和表面等离振子共振确定了新的单体复合物,以及两个DB2277与某些序列的意外结合。通过计算分析来识别实验DNA内在的固有微结构差异,以了解识别的分子基础。这些发现强调了DNA小沟微结构对于序列特异性识别的关键性质,并为设计合成小分子以有效调节基因表达提供了新途径。

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