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Combined single-molecule manipulation and localization for the study of lac Repressor ID-diffusion along DNA

机译:组合单分子操纵与定位在DNA沿着DNA研究Lac压缩机Id-扩散的研究

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The maintenance of intact genetic information, as well as the deployment of transcription for specific sets of genes, critically rely on a family of proteins interacting with DNA and recognizing specific sequences or features. The mechanisms by which these proteins search for target DNA are the subject of intense investigations employing a variety of methods in biology. A large interest in these processes stems from the faster-than-diffusion association rates, explained in current models by a combination of 3D and ID diffusion. Here, we describe the combination of optical tweezers and single molecule fluorescence detection for the study of protein-DNA interaction. The method offers the opportunity of investigating interactions occurring in solution (thus avoiding problems due to closeby surfaces as in other single molecule methods), controlling the DNA extension and tracking interaction dynamics as a function of both mechanical parameters and DNA sequence.
机译:维持完整的遗传信息,以及对特定基因组转录的部署,依赖于与DNA相互作用的蛋白质系列并识别特定序列或特征。这些蛋白质搜索靶DNA的机制是采用各种生物学方法的强烈调查的主题。对这些过程的较大兴趣源于更快的扩散关联率,通过3D和ID扩散的组合在当前模型中解释。在这里,我们描述了光学镊子和单分子荧光检测的组合,用于研究蛋白质-DNA相互作用。该方法提供了在溶液中进行的相互作用的机会(从而避免由于其他单一分子方法而导致的表面),控制DNA延伸和跟踪相互作用动态作为机械参数和DNA序列的函数。

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