Publication | Closed Access
Toward Larger DNA Origami
188
Citations
39
References
2014
Year
EngineeringBiomimetic MaterialsGeneticsDna AnalysisMolecular BiologyBiofabricationFoldable StructureDna OrigamiStructural Dna NanotechnologyDna Origami SizeDna NanotechnologyMaterials FabricationGenome EngineeringDna ComputingBiological NanomaterialsNanomanufacturingOligonucleotideDna ReplicationBiopolymersMolecular EngineeringBiomolecular EngineeringNatural SciencesSelf-assemblyGenetic EngineeringSynthetic BiologyNanofabricationGenome Editing
Structural DNA nanotechnology, and specifically scaffolded DNA origami, is rapidly developing as a versatile method for bottom-up fabrication of novel nanometer-scale materials and devices. However, lengths of conventional single-stranded scaffolds, for example, 7,249-nucleotide circular genomic DNA from the M13mp18 phage, limit the scales of these uniquely addressable structures. Additionally, increasing DNA origami size generates the cost burden of increased staple-strand synthesis. We addressed this 2-fold problem by developing the following methods: (1) production of the largest to-date biologically derived single-stranded scaffold using a λ/M13 hybrid virus to produce a 51 466-nucleotide DNA in a circular, single-stranded form and (2) inexpensive DNA synthesis via an inkjet-printing process on a chip embossed with functionalized micropillars made from cyclic olefin copolymer. We have experimentally demonstrated very efficient assembly of a 51-kilobasepair origami from the λ/M13 hybrid scaffold folded by chip-derived staple strands. In addition, we have demonstrated two-dimensional, asymmetric origami sheets with controlled global curvature such that they land on a substrate in predictable orientations that have been verified by atomic force microscopy.
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