DNA Nanostructure-Guided Assembly of Proteins into Programmable Shapes

The development of methods to synthesize protein oligomers with precisely controlled number and configuration of components will enable artificial protein complexes and nanostructures with diverse biological and medical applications. Using DNA hybridization to link protein-DNA conjugates provides for a programmability that can be difficult to achieve with other methods, such as engineering multiple orthogonal protein-protein interfaces. However, it is still difficult to construct well-defined protein assemblies, and the challenge is magnified if only a single type of building block is used. To overcome this hurdle, we use a DNA origami as an “assembler” to guide the linking of protein-DNA conjugates using a series of oligonucleotide hybridization and displacement operations. We constructed several isomeric protein nanostructures on a DNA origami platform by using a C3-symmetric building block comprised of a protein trimer modified with DNA handles. By changing the number of protein-DNA building blocks attached to the origami, and the sequence of the linking and displacement strands added, we were able to produce dimers, two types of trimer structures, and three types of tetramer assemblies. Our approach expands the scope for the precise design and assembly of protein-based nanostructures, and will enable the formulation of functional protein complexes with stoichiometric and geometric control. ### Competing Interest Statement The authors have declared no competing interest.