The use of different condensing and phosphorylating agents in conjunction with oxygen-nucleophilic catalysts, such as 4-substituted derivatives of pyridine N-oxide and quinoline N-oxide, leads to a dramatic increase of the rate of the phosphotriester bond formation and minimizes the amount of by-products caused by the modification of heterocyclic bases. The application of these catalysts to the solid-phase oligonucleotide synthesis allows to reduce the time needed for the performance of one elongation cycle on a polymer support to 10 min. © 1985 IRL Press Limited.
CITATION STYLE
Efimov, V. A., Chakhmakhcheva, O. G., & Ovchinnikov, Y. A. (1985). Improved rapid phosphotriester synthesis of oligodeoxyribonueleotides using oxygen-nucleoplillic cataiysts. Nucleic Acids Research, 13(10), 3651–3666. https://doi.org/10.1093/nar/13.10.3651
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