Conformational flexibility facilitates self-assembly of complex DNA nanostructures
- Chuan Zhang*,
- Min Su†,
- Yu He*,
- Xin Zhao†,
- Ping-an Fang†,
- Alexander E. Ribbe*,
- Wen Jiang†, and
- Chengde Mao*,‡
- *Department of Chemistry and
- †Markey Center for Structural Biology and Department of Biological Sciences, Purdue University, West Lafayette, IN 47907
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Edited by Hao Yan, Arizona State University, Tempe, AZ, and accepted by the Editorial Board May 28, 2008 (received for review April 23, 2008)
Abstract
Molecular self-assembly is a promising approach to the preparation of nanostructures. DNA, in particular, shows great potential to be a superb molecular system. Synthetic DNA molecules have been programmed to assemble into a wide range of nanostructures. It is generally believed that rigidities of DNA nanomotifs (tiles) are essential for programmable self-assembly of well defined nanostructures. Recently, we have shown that adequate conformational flexibility could be exploited for assembling 3D objects, including tetrahedra, dodecahedra, and buckyballs, out of DNA three-point star motifs. In the current study, we have integrated tensegrity principle into this concept to assemble well defined, complex nanostructures in both 2D and 3D. A symmetric five-point-star motif (tile) has been designed to assemble into icosahedra or large nanocages depending on the concentration and flexibility of the DNA tiles. In both cases, the DNA tiles exhibit significant flexibilities and undergo substantial conformational changes, either symmetrically bending out of the plane or asymmetrically bending in the plane. In contrast to the complicated natures of the assembled structures, the approach presented here is simple and only requires three different component DNA strands. These results demonstrate that conformational flexibility could be explored to generate complex DNA nanostructures. The basic concept might be further extended to other biomacromolecular systems, such as RNA and proteins.
Footnotes
- ‡To whom correspondence should be addressed at: 560 Oval Drive, West Lafayette, IN 47907. E-mail: mao{at}purdue.edu
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Author contributions: C.Z., W.J., and C.M. designed research; C.Z., M.S., and Y.H. performed research; C.Z., M.S., Y.H., X.Z., P.-a.F., A.E.R., W.J., and C.M. analyzed data; and C.Z. and C.M. wrote the paper.
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The authors declare no conflict of interest.
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This article is a PNAS Direct Submission. H.Y. is a guest editor invited by the Editorial Board.
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This article contains supporting information online at www.pnas.org/cgi/content/full/0803841105/DCSupplemental.
- © 2008 by The National Academy of Sciences of the USA





