Sequence-specific artificial ribonucleases. I. Bis-imidazole-containing oligonucleotide conjugates prepared using precursor-based strategy

doi:10.1093/nar/gkh702

Nucleic Acids Research 2004 32(13):3887-3897; doi:10.1093/nar/gkh702

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Published online 23 July 2004

Sequence-specific artificial ribonucleases. I. Bis-imidazole-containing oligonucleotide conjugates prepared using precursor-based strategy

Natalia G. Beloglazova, Martin M. Fabani¹, Marina A. Zenkova^*, Elena V. Bichenkova¹, Nikolai N. Polushin², Vladimir V. Sil'nikov, Kenneth T. Douglas¹ and Valentin V. Vlassov

Institute of Chemical Biology and Fundamental Medicine, Siberian Division of the Russian Academy of Sciences, Novosibirsk 630090, Russian Federation, ¹ Wolfson Centre for Rational Design of Molecular Diagnostics, School of Pharmacy and Pharmaceutical Sciences, University of Manchester, Manchester M13 9PL, UK and ² Fidelity Systems Inc., 7961 Cessna Avenue, Gaithersburg, MD 20879, USA

^* To whom correspondence should be addressed. Tel: +7 3832 333761; Fax: +7 3832 333677; Email: marzen{at}niboch.nsc.ru

Received May 21, 2004; Revised and Accepted June 24, 2004

Antisense oligonucleotide conjugates, bearing constructs withtwo imidazole residues, were synthesized using a precursor-basedtechnique employing post-synthetic histamine functionalizationof oligonucleotides bearing methoxyoxalamido precursors at the5'-termini. The conjugates were assessed in terms of their cleavageactivities using both biochemical assays and conformationalanalysis by molecular modelling. The oligonucleotide part ofthe conjugates was complementary to the T-arm of yeast tRNA^Phe(44–60 nt) and was expected to deliver imidazole groupsnear the fragile sequence C₆₁-ACA-G₆₅ of the tRNA. The conjugatesshowed ribonuclease activity at neutral pH and physiologicaltemperature resulting in complete cleavage of the target RNA,mainly at the C₆₃–A₆₄ phosphodiester bond. For some constructs,cleavage was completed within 1–2 h under optimal conditions.Molecular modelling was used to determine the preferred orientation(s)of the cleaving group(s) in the complexes of the conjugateswith RNA target. Cleaving constructs bearing two imidazole residueswere found to be conformationally highly flexible, adoptingno preferred specific conformation. No interactions other thancomplementary base pairing between the conjugates and the targetwere found to be the factors stabilizing the ‘active’cleaving conformation(s).

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