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Isothermal hybridization kinetics of DNA assembly of two-dimensional DNA origami

机译:二维DNA折纸的DNA组装等温杂交动力学

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The Watson-Crick base-pairing with specificity and predictability makes DNA molecules suitable for building versatile nanoscale structures and devices, and the DNA origami method enables researchers to incorporate more complexities into DNA-based devices. Thermally controlled atomic force microscopy in combination with nanomechanical spectroscopy with forces controlled in the pico Newton (pN) range as a novel technique is introduced to directly investigate the kinetics of multistrand DNA hybridization events on DNA origami nanopores under defined isothermal conditions. For the synthesis of DNA nanostructures under isothermal conditions at 60 °C, a higher hybridization rate, fewer defects, and a higher stability are achieved compared to room-temperature studies. By quantifying the assembly times for filling pores in origami structures at several constant temperatures, the fill factors show a consistent exponential increase over time. Furthermore, the local hybridization rate can be accelerated by adding a higher concentration of the staples. The new insight gained on the kinetics of staple-scaffold hybridization on the synthesis of two dimensional DNA origami structures may open up new routes and ideas for designing DNA assembly systems with increased potential for their application.
机译:具特异性和可预测性的Watson-Crick碱基对使DNA分子适合构建通用的纳米级结构和设备,而DNA折纸方法使研究人员能够将更多复杂性纳入基于DNA的设备中。引入了热控制原子力显微镜技术和纳米机械光谱学,将力控制在皮克牛顿(pN)范围内,将其作为一种新技术直接研究在限定的等温条件下DNA折纸纳米孔上多链DNA杂交事件的动力学。与室温研究相比,在等温条件下于60°C合成DNA纳米结构时,可获得更高的杂交速率,更少的缺陷和更高的稳定性。通过量化在几个恒定温度下填充折纸结构中的孔的组装时间,填充因子显示出随时间呈指数增长的趋势。此外,可以通过添加较高浓度的钉来加速局部杂交速率。在合成二维DNA折纸结构的钉书架杂交动力学方面获得的新见解可能会为设计具有更大应用潜力的DNA组装系统开辟新途径和新思路。

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