An LNA-amide modification that enhances the cell uptake and activity of phosphorothioate exon-skipping oligonucleotides

Author:

Baker Ysobel R.ORCID,Thorpe CameronORCID,Chen Jinfeng,Poller Laura M.ORCID,Cox LinaORCID,Kumar Pawan,Lim Wooi F.ORCID,Lie Lillian,McClorey Graham,Epple SvenORCID,Singleton Daniel,McDonough Michael A.ORCID,Hardwick Jack S.ORCID,Christensen Kirsten E.ORCID,Wood Matthew J. A.ORCID,Hall James P.ORCID,El-Sagheer Afaf H.ORCID,Brown TomORCID

Abstract

AbstractOligonucleotides that target mRNA have great promise as therapeutic agents for life-threatening conditions but suffer from poor bioavailability, hence high cost. As currently untreatable diseases come within the reach of oligonucleotide therapies, new analogues are urgently needed to address this. With this in mind we describe reduced-charge oligonucleotides containing artificial LNA-amide linkages with improved gymnotic cell uptake, RNA affinity, stability and potency. To construct such oligonucleotides, five LNA-amide monomers (A, T, C, 5mC and G), where the 3′-OH is replaced by an ethanoic acid group, are synthesised in good yield and used in solid-phase oligonucleotide synthesis to form amide linkages with high efficiency. The artificial backbone causes minimal structural deviation to the DNA:RNA duplex. These studies indicate that splice-switching oligonucleotides containing LNA-amide linkages and phosphorothioates display improved activity relative to oligonucleotides lacking amides, highlighting the therapeutic potential of this technology.

Funder

RCUK | Biotechnology and Biological Sciences Research Council

Publisher

Springer Science and Business Media LLC

Subject

General Physics and Astronomy,General Biochemistry, Genetics and Molecular Biology,General Chemistry,Multidisciplinary

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