Computational approaches toward the design of pools for the in vitro selection of complex aptamers

  1. Frank Dehne1
  1. 1School of Computer Science, Carleton University, Ottawa, Ontario K1S 5B6, Canada
  2. 2Department of Chemistry, Carleton University, Ottawa, Ontario K1S 5B6, Canada
  3. 3Department of Biology, Carleton University, Ottawa, Ontario K1S 5B6, Canada
  4. 4Department of Systems and Computer Engineering, Carleton University, Ottawa, Ontario K1S 5B6, Canada
  1. 5 These authors contributed equally to this work.

Abstract

It is well known that using random RNA/DNA sequences for SELEX experiments will generally yield low-complexity structures. Early experimental results suggest that having a structurally diverse library, which, for instance, includes high-order junctions, may prove useful in finding new functional motifs. Here, we develop two computational methods to generate sequences that exhibit higher structural complexity and can be used to increase the overall structural diversity of initial pools for in vitro selection experiments. Random Filtering selectively increases the number of five-way junctions in RNA/DNA pools, and Genetic Filtering designs RNA/DNA pools to a specified structure distribution, whether uniform or otherwise. We show that using our computationally designed DNA pool greatly improves access to highly complex sequence structures for SELEX experiments (without losing our ability to select for common one-way and two-way junction sequences).

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Footnotes

  • Reprint requests to: Maria C. Derosa, Department of Chemistry, Carleton University, Ottawa, Ontario K1S 5B6, Canada; e-mail: maria_derosa{at}carleton.ca; or Frank Dehne, School of Computer Science, Carleton University, Ottawa, Ontario K1S 5B6, Canada; e-mail: frank{at}dehne.net; fax: (613) 520-4334.

  • Article published online ahead of print. Article and publication date are at http://www.rnajournal.org/cgi/doi/10.1261/rna.2102210.

  • Received January 22, 2010.
  • Accepted August 13, 2010.
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