Nucleic Acids Research

Nucleic Acids Research 2006 34(8):2166-2172; doi:10.1093/nar/gkl176

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Published online 28 April 2006

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Article

Deoxyribozymes that recode sequence information

Jeffrey J. Tabor¹, Matthew Levy¹ and Andrew D. Ellington^1,2,*

¹ Center for Systems and Synthetic Biology and Institute for Cell and Molecular Biology, University of Texas at Austin Austin, TX 78712, USA ² Department of Chemistry and Biochemistry, University of Texas at Austin Austin, TX 78712, USA

^*To whom correspondence should be addressed. Tel: 1 512 471 6445; Fax: 1 512 471 7014; Email: andy.ellington{at}mail.utexas.edu

Received January 25, 2006. Revised March 21, 2006. Accepted March 21, 2006.

Allosteric nucleic acid ligases have been used previously to transform analyte-binding into the formation of oligonucleotide templates that can be amplified and detected. We have engineered binary deoxyribozyme ligases whose two components are brought together by bridging oligonucleotide effectors. The engineered ligases can ‘read’ one sequence and then ‘write’ (by ligation) a separate, distinct sequence, which can in turn be uniquely amplified. The binary deoxyribozymes show great specificity, can discriminate against a small number of mutations in the effector, and can read and recode DNA information with high fidelity even in the presence of excess obscuring genomic DNA. In addition, the binary deoxyribozymes can read non-natural nucleotides and write natural sequence information. The binary deoxyribozyme ligases could potentially be used in a variety of applications, including the detection of single nucleotide polymorphisms in genomic DNA or the identification of short nucleic acids such as microRNAs.

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