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The diversity of SNCA transcripts in neurons, and its impact on antisense oligonucleotide therapeutics

Output Details

The role of the SNCA gene locus in driving Parkinson’s disease (PD) through rare and common genetic variation is well-recognized, but the transcriptional diversity of SNCA in vulnerable cell types remains unclear. We performed SNCA long-read RNA sequencing in human dopaminergic neurons and show that annotated SNCA transcripts account for only 5% of expression. Rather, the majority of expression (75%) at the SNCA locus originates from transcripts with alternative 5’ and 3’ untranslated regions. Importantly, 10% originates from transcripts encoding open reading frames not previously annotated, which are translated and detectable in human postmortem brain. Defining the 3’ untranslated regions enabled the rational design of antisense oligonucleotides targeting the majority of SNCA transcripts, leading to the effective reversal of PD pathology, including protein aggregation, mitochondrial dysfunction, and toxicity. Resolving the complexity of the SNCA transcriptional landscape impacts RNA therapies and highlights differences in protein isoforms and their contribution to disease.
Tags
  • SNCA
  • Transcripts

Meet the Authors

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    James Evans, MSc

    Key Personnel: Team Wood

    University College London

  • Emil Gustavsson, PhD

    Key Personnel: Team Wood Team Hardy

    University College London

  • User avatar fallback logo

    Ivan Doykov

    External Collaborator

  • User avatar fallback logo

    David Murphy, MSc

    Key Personnel: Team Wood

    University College London

  • Gurvir Virdi, MSc

    Key Personnel: Team Wood

    The Francis Crick Institute

  • User avatar fallback logo

    Joanne Lachica, MD

    Key Personnel: Team Wood

    University College London

  • User avatar fallback logo

    Alexander Röntgen, MSc

    Key Personnel: Team Wood

    University of Cambridge

  • User avatar fallback logo

    Mhd Hussein Murtada

    External Collaborator

  • User avatar fallback logo

    Chun Wei Pang

    External Collaborator

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    Hannah Macpherson, MSc

    Key Personnel: Team Wood

    University College London

  • Anna Wernick, BSc

    Key Personnel: Team Hardy Team Wood

    University College London

  • Christina Toomey, PhD

    Key Personnel: Team Wood

    University College London

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    Dilan Athauda

    External Collaborator

  • Minee Choi, PhD

    Key Personnel: Team Wood

    The Francis Crick Institute

  • John Hardy, PhD

    Lead PI (Core Leadership): Team Hardy

    University College London

  • Nicholas Wood, PhD

    Lead PI (Core Leadership): Team Wood

    University College London

  • Michele Vendruscolo, PhD

    Co-PI (Core Leadership): Team Wood

    University of Cambridge

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    Kevin Mills

    External Collaborator

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    Wendy Heywood

    External Collaborator

  • Mina Ryten

    Co-PI (Core Leadership): Team Hardy Team Wood

    University College London

  • Sonia Gandhi, PhD

    Co-PI (Core Leadership): Team Wood

    University College London

Aligning Science Across Parkinson's
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