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Directing folding pathways for multi-component DNA origami nanostructures with complex topology

机译:指导具有复杂拓扑结构的多组分DNA折纸纳米结构的折叠途径

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Molecular self-assembly has become a well-established technique to design complex nanostructures and hierarchical mesoscale assemblies. The typical approach is to design binding complementarity into nucleotide or amino acid sequences to achieve the desired final geometry. However, with an increasing interest in dynamic nanodevices, the need to design structures with motion has necessitated the development of multi-component structures. While this has been achieved through hierarchical assembly of similar structural units, here we focus on the assembly of topologically complex structures, specifically with concentric components, where post-folding assembly is not feasible. We exploit the ability to direct folding pathways to program the sequence of assembly and present a novel approach of designing the strand topology of intermediate folding states to program the topology of the final structure, in this case a DNA origami slider structure that functions much like a piston-cylinder assembly in an engine. The ability to program the sequence and control orientation and topology of multi-component DNA origami nanostructures provides a foundation for a new class of structures with internal and external moving parts and complex scaffold topology. Furthermore, this work provides critical insight to guide the design of intermediate states along a DNA origami folding pathway and to further understand the details of DNA origami self-assembly to more broadly control folding states and landscapes.
机译:分子自组装已成为设计复杂的纳米结构和分层中尺度组装的公认技术。典型的方法是设计成核苷酸或氨基酸序列的结合互补性以获得所需的最终几何形状。然而,随着人们对动态纳米器件的兴趣日益浓厚,对设计具有运动性的结构的需求使得必须开发多组件结构。尽管这是通过类似结构单元的分层组装来实现的,但在此我们重点关注拓扑复杂的结构的组装,特别是同心组件的组装,而后折叠组装则不可行。我们利用引导折叠路径来编程装配顺序的能力,并提出了一种设计中间折叠状态的链拓扑结构以编程最终结构的拓扑结构的新方法,在这种情况下,DNA折纸滑块结构的功能很像发动机中的活塞缸组件。对多组分DNA折纸纳米结构的序列,控制方向和拓扑进行编程的能力为具有内部和外部移动部件以及复杂支架拓扑的新型结构提供了基础。此外,这项工作提供了重要的见识,可指导DNA折纸折叠路径中中间状态的设计,并进一步理解DNA折纸自组装的细节,以更广泛地控制折叠状态和景观。

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