Oligonucleotide circularization by template-directed chemical ligation

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Abstract

An efficient method for producing the covalent closure of oligonucleotides on complementary templates by the action of BrCN was developed. A rational design of linear precursor oligonucleotides was studied, and the effect of factors such as oligonucleotide concentration and oligomer-template length ratio was evaluated. The efficiency of circularization was shown to correlate well with the secondary structure of the precursor oligomer (as predicted by a simple computer analysis), hairpinlike structures bearing free termini clearly favouring the circularization reaction. A novel idea, consisting of the incorporation of non-nucleotide insertions in the precursor oligomer (namely, 1,2-dideoxy-D-ribofuranose residues), may render this method universal and highly effective. An original set of assays was developed to confirm the circular structure of the covalently closed oligonucleotides. © 1993 Oxford University Press.

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CITATION STYLE

APA

Dolinnaya, N. G., Blumenfeld, M., Merenkova, I. N., Oretskaya, T. S., Krynetskaya, N., Ivanovskaya, M. G., … Shabarova, Z. A. (1993). Oligonucleotide circularization by template-directed chemical ligation. Nucleic Acids Research, 21(23), 5403–5407. https://doi.org/10.1093/nar/21.23.5403

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