Antisense oligonucleotide mediated terminal intron retention of the SMN2 transcript

L.L. Flynn; C. Mitrpant; I.L. Pitout; S. Fletcher; S.D. Wilton

doi:10.1016/j.omtn.2018.01.011

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Antisense oligonucleotide mediated terminal intron retention of the SMN2 transcript

Journal article

Open access

Peer reviewed

Antisense oligonucleotide mediated terminal intron retention of the SMN2 transcript

L.L. Flynn, C. Mitrpant, I.L. Pitout, S. Fletcher and S.D. Wilton

Molecular Therapy - Nucleic Acids, Vol.11, pp.91-102

2018

DOI: https://doi.org/10.1016/j.omtn.2018.01.011

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Abstract

The severe childhood disease spinal muscular atrophy (SMA) arises from the homozygous loss of the survival motor neuron 1 gene (SMN1). A homologous gene potentially encoding an identical protein, SMN2 can partially compensate for the loss of SMN1, however the exclusion of a critical exon in the coding region during mRNA maturation results in insufficient levels of functional protein. The rate of transcription is known to influence the alternative splicing of gene transcripts, with a fast transcription rate correlating to an increase in alternative splicing. Conversely, a slower transcription rate is more likely to result in the inclusion of all exons in the transcript. Targeting SMN2 with antisense oligonucleotides to influence the processing of terminal exon 8 could be a way to slow transcription and induce the inclusion of exon 7. Interestingly, following oligomer treatment of SMA patient fibroblasts, we observed the inclusion of exon 7 as well as intron 7 in the transcript. Since the normal termination codon is located in exon 7, this exon/intron7-SMN2 transcript should encode the normal protein, and only carry a longer 3´ untranslated region. Further studies showed the extra 3´UTR length contained a number of regulatory motifs that modify transcript and protein regulation, leading to translational repression of SMN. While unlikely to provide therapeutic benefit for spinal muscular atrophy patients, this novel technique for gene regulation could provide another avenue for the repression of undesirable gene expression in a variety of other diseases.

Details

Title: Antisense oligonucleotide mediated terminal intron retention of the SMN2 transcript
Authors/Creators: L.L. Flynn (Author/Creator)
C. Mitrpant (Author/Creator)
I.L. Pitout (Author/Creator)
S. Fletcher (Author/Creator)
S.D. Wilton (Author/Creator)
Publication Details: Molecular Therapy - Nucleic Acids, Vol.11, pp.91-102
Publisher: Elsevier
Identifiers: 991005544314807891
Copyright: © 2018 The Authors.
Murdoch Affiliation: Centre for Comparative Genomics
Language: English
Resource Type: Journal article

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Collaboration types: Domestic collaboration; International collaboration
Citation topics: 1 Clinical & Life Sciences; 1.54 Molecular & Cell Biology - Genetics; 1.54.469 Alternative Splicing
Web Of Science research areas: Medicine, Research & Experimental
ESI research areas: Biology & Biochemistry