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单颗粒跟踪和超分辨率成像在膜辅助停止和游走扩散以及 DNA 折纸的晶格组装中的应用。

Single Particle Tracking and Super-Resolution Imaging of Membrane-Assisted Stop-and-Go Diffusion and Lattice Assembly of DNA Origami.

机构信息

Faculty of Physics and Center for NanoScience , Ludwig-Maximilians-Universität , München 80539 , Germany.

Max Planck Institute of Biochemistry , Martinsried 82152 , Germany.

出版信息

ACS Nano. 2019 Feb 26;13(2):996-1002. doi: 10.1021/acsnano.8b04631. Epub 2019 Jan 7.

DOI:10.1021/acsnano.8b04631
PMID:30588792
Abstract

DNA nanostructures offer the possibility to mimic functional biological membrane components due to their nanometer-precise shape configurability and versatile biochemical functionality. Here we show that the diffusional behavior of DNA nanostructures and their assembly into higher order membrane-bound lattices can be controlled in a stop-and-go manner and that the process can be monitored with super-resolution imaging. The DNA structures are transiently immobilized on glass-supported lipid bilayers by changing the mono- and divalent cation concentrations of the surrounding buffer. Using DNA points accumulation for imaging in nanoscale topography (DNA-PAINT) super-resolution microscopy, we confirm the fixation of DNA origami structures with different shapes. On mica-supported lipid bilayers, in contrast, we observe residual movement. By increasing the concentration of NaCl and depleting MgCl, a large fraction of DNA structures restarts to diffuse freely on both substrates. After addition of a set of oligonucleotides that enables three Y-shaped monomers to assemble into a three-legged shape (triskelion), the triskelions can be stopped and super-resolved. Exchanging buffer and adding another set of oligonucleotides triggers the triskelions to diffuse and assemble into hexagonal 2D lattices. This stop-and-go imaging technique provides a way to control and observe the diffusional behavior of DNA nanostructures on lipid membranes that could also lead to control of membrane-associated cargos.

摘要

DNA 纳米结构由于其纳米级精确的形状可变性和多功能的生化功能,提供了模拟功能性生物膜成分的可能性。在这里,我们展示了 DNA 纳米结构的扩散行为及其在更高阶的膜结合晶格中的组装可以以停止-启动方式进行控制,并且可以通过超分辨率成像进行监测。通过改变周围缓冲液中的单价和二价阳离子浓度,DNA 结构可以在玻璃支持的脂质双层上短暂固定。使用 DNA 点积累成像纳米形貌学(DNA-PAINT)超分辨率显微镜,我们证实了不同形状的 DNA 折纸结构的固定。相比之下,在云母支持的脂质双层上,我们观察到残留的运动。通过增加 NaCl 的浓度并耗尽 MgCl2,大部分 DNA 结构在两种基质上重新开始自由扩散。在添加一组能够使三个 Y 形单体组装成三足形(三脚架)的寡核苷酸后,三脚架可以被停止并进行超分辨。交换缓冲液并添加另一组寡核苷酸会触发三脚架扩散并组装成六边形 2D 晶格。这种停止-启动成像技术为控制和观察脂质膜上 DNA 纳米结构的扩散行为提供了一种方法,这也可能导致对膜相关载体的控制。

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