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利用单分子荧光技术开发 DNA 纳米技术。

Developing DNA nanotechnology using single-molecule fluorescence.

机构信息

Department of Chemistry and the Ilse Katz Institute for Nanoscale Science and Technology, Ben-Gurion University of the Negev , Beer Sheva, 84105, Israel.

出版信息

Acc Chem Res. 2014 Jun 17;47(6):1789-98. doi: 10.1021/ar500027d. Epub 2014 May 14.

Abstract

CONSPECTUS

An important effort in the DNA nanotechnology field is focused on the rational design and manufacture of molecular structures and dynamic devices made of DNA. As is the case for other technologies that deal with manipulation of matter, rational development requires high quality and informative feedback on the building blocks and final products. For DNA nanotechnology such feedback is typically provided by gel electrophoresis, atomic force microscopy (AFM), and transmission electron microscopy (TEM). These analytical tools provide excellent structural information; however, usually they do not provide high-resolution dynamic information. For the development of DNA-made dynamic devices such as machines, motors, robots, and computers this constitutes a major problem. Bulk-fluorescence techniques are capable of providing dynamic information, but because only ensemble averaged information is obtained, the technique may not adequately describe the dynamics in the context of complex DNA devices. The single-molecule fluorescence (SMF) technique offers a unique combination of capabilities that make it an excellent tool for guiding the development of DNA-made devices. The technique has been increasingly used in DNA nanotechnology, especially for the analysis of structure, dynamics, integrity, and operation of DNA-made devices; however, its capabilities are not yet sufficiently familiar to the community. The purpose of this Account is to demonstrate how different SMF tools can be utilized for the development of DNA devices and for structural dynamic investigation of biomolecules in general and DNA molecules in particular. Single-molecule diffusion-based Förster resonance energy transfer and alternating laser excitation (sm-FRET/ALEX) and immobilization-based total internal reflection fluorescence (TIRF) techniques are briefly described and demonstrated. To illustrate the many applications of SMF to DNA nanotechnology, examples of SMF studies of DNA hairpins and Holliday junctions and of the interactions of DNA strands with DNA origami and origami-related devices such as a DNA bipedal motor are provided. These examples demonstrate how SMF can be utilized for measurement of distances and conformational distributions and equilibrium and nonequilibrium kinetics, to monitor structural integrity and operation of DNA devices, and for isolation and investigation of minor subpopulations including malfunctioning and nonreactive devices. Utilization of a flow-cell to achieve measurements of dynamics with increased time resolution and for convenient and efficient operation of DNA devices is discussed briefly. We conclude by summarizing the various benefits provided by SMF for the development of DNA nanotechnology and suggest that the method can significantly assist in the design and manufacture and evaluation of operation of DNA devices.

摘要

概述

DNA 纳米技术领域的一个重要努力集中在 DNA 分子结构和动态器件的合理设计和制造上。与其他涉及物质操纵的技术一样,合理的发展需要对构建块和最终产品进行高质量和信息丰富的反馈。对于 DNA 纳米技术,这种反馈通常由凝胶电泳、原子力显微镜 (AFM) 和透射电子显微镜 (TEM) 提供。这些分析工具提供了极好的结构信息;然而,它们通常不能提供高分辨率的动态信息。对于 DNA 制造的动态器件(如机器、马达、机器人和计算机)的发展,这构成了一个主要问题。体荧光技术能够提供动态信息,但由于只能获得整体平均信息,因此该技术可能无法充分描述复杂 DNA 器件背景下的动力学。单分子荧光 (SMF) 技术提供了独特的功能组合,使其成为指导 DNA 器件开发的绝佳工具。该技术已越来越多地应用于 DNA 纳米技术,特别是用于分析 DNA 器件的结构、动力学、完整性和操作;然而,其功能尚未为该领域所熟知。本综述旨在展示如何利用不同的 SMF 工具来开发 DNA 器件,并研究一般生物分子和特定 DNA 分子的结构动态。简要描述并演示了基于单分子扩散的Förster 共振能量转移和交替激光激发 (sm-FRET/ALEX) 和基于固定化的全内反射荧光 (TIRF) 技术。为了说明 SMF 对 DNA 纳米技术的广泛应用,提供了 SMF 研究 DNA 发夹和 Holliday 结以及 DNA 链与 DNA 折纸和折纸相关器件(如 DNA 双足马达)相互作用的实例。这些实例表明,SMF 可用于测量距离和构象分布以及平衡和非平衡动力学,监测 DNA 器件的结构完整性和操作,并分离和研究包括故障和非反应性器件在内的少数亚群。简要讨论了使用流动池实现具有更高时间分辨率的动力学测量以及方便和高效操作 DNA 器件的问题。我们最后总结了 SMF 为 DNA 纳米技术发展提供的各种好处,并提出该方法可以显著协助 DNA 器件的设计、制造和操作评估。

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