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单分子-DNA复合物中结合机制的鉴定

Identification of binding mechanisms in single molecule-DNA complexes.

作者信息

Eckel Rainer, Ros Robert, Ros Alexandra, Wilking Sven David, Sewald Norbert, Anselmetti Dario

机构信息

Experimental Biophysics and Applied Nanosciences, Faculty of Physics, Bielefeld University, 33615 Bielefeld, Germany.

出版信息

Biophys J. 2003 Sep;85(3):1968-73. doi: 10.1016/S0006-3495(03)74624-4.

Abstract

Changes in the elastic properties of single deoxyribonucleic acid (DNA) molecules in the presence of different DNA-binding agents are identified using atomic force microscope single molecule force spectroscopy. We investigated the binding of poly(dG-dC) dsDNA with the minor groove binder distamycin A, two supposed major groove binders, an alpha-helical and a 3(10)-helical peptide, the intercalants daunomycin, ethidium bromide and YO, and the bis-intercalant YOYO. Characteristic mechanical fingerprints in the overstretching behavior of the studied single DNA-ligand complexes were observed allowing the distinction between different binding modes. Docking of ligands to the minor or major groove of DNA has the effect that the intramolecular B-S transition remains visible as a distinct plateau in the force-extension trace. By contrast, intercalation of small molecules into the double helix is characterized by the vanishing of the B-S plateau. These findings lead to the conclusion that atomic force microscope force spectroscopy can be regarded as a single molecule biosensor and is a potent tool for the characterization of binding motives of small ligands to DNA.

摘要

利用原子力显微镜单分子力谱技术,识别了在不同DNA结合剂存在下单个脱氧核糖核酸(DNA)分子弹性特性的变化。我们研究了聚(dG-dC)双链DNA与小沟结合剂偏端霉素A、两种假定的大沟结合剂(一种α-螺旋肽和一种3(10)-螺旋肽)、嵌入剂柔红霉素、溴化乙锭和YO以及双嵌入剂YOYO的结合情况。在研究的单个DNA-配体复合物的过度拉伸行为中观察到了特征性的机械指纹,从而能够区分不同的结合模式。配体与DNA小沟或大沟的对接会使分子内B-S转变在力-伸长曲线上作为一个明显的平台保持可见。相比之下,小分子插入双螺旋的特征是B-S平台消失。这些发现得出结论,原子力显微镜力谱可被视为一种单分子生物传感器,是表征小配体与DNA结合模式的有力工具。

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