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Alternate PNA-DNA chimeras (PNA-DNA)n: Synthesis, binding properties and biological activity

✍ Scribed by Loredana Moggio; Alessandra Romanelli; Roberto Gambari; Nicoletta Bianchi; Monica Borgatti; Enrica Fabbri; Irene Mancini; Benedetto di Blasio; Carlo Pedone; Anna Messere


Publisher
Wiley (John Wiley & Sons)
Year
2007
Tongue
English
Weight
222 KB
Volume
88
Category
Article
ISSN
0006-3525

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✦ Synopsis


Peptide nucleic acids (PNAs) are oligonucleotide mimics in which the sugar-phosphate backbone has been replaced by a pseudo-peptide backbone. Among PNA-based molecules, PNA-DNA conjugates characterized by tracts of DNA bound to N and/or C terminus of PNA are very soluble in aqueous media, are able to recognize exclusively single strands of DNA and RNA in antiparallel fashion, activate RNAse H, bind to transcription factors and are more stable than DNA to nucleases degradation. Very little information is available on chimeras constituted of alternating monomers of PNA and DNA. In this article, we describe a simple fully automated strategy for the synthesis of 6-mer and 10-mer alternate PNA-DNA chimeras consisting of polythymine oligomers, stability assays in fetal calf serum, UV and CD studies of the single strand alternate chimeras and of alternate chimera/DNA and alternate chimera/RNA duplexes. Evidences supporting the formation of duplex hybrids were found. Furthermore, the ability of forming Hoogsteen base pairing with duplex DNA was investigated. Finally, we tested the ability of the PNA-DNA alternates in (a) interfering with reverse transcription of eukaryotic mRNA and (b) inhibiting DNA-protein interactions.


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## Abstract A new synthetic strategy to get the PNA–3β€²DNA linker with the monomethoxytrityl (Mmt) group as temporary protection of the backbone to be used for the synthesis of PNA/DNA chimeras was employed and a convenient strategy to obtain Mmt PNA monomers was developed. The synthetic strategies