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Determination of RNA structural diversity and its role in HIV-1 RNA splicing

Author

Listed:
  • Phillip J. Tomezsko

    (Whitehead Institute for Biomedical Research
    Harvard Medical School
    Brigham and Women’s Hospital)

  • Vincent D. A. Corbin

    (Walter and Eliza Hall Institute
    The University of Melbourne)

  • Paromita Gupta

    (Whitehead Institute for Biomedical Research)

  • Harish Swaminathan

    (Whitehead Institute for Biomedical Research)

  • Margalit Glasgow

    (Whitehead Institute for Biomedical Research
    Massachusetts Institute of Technology)

  • Sitara Persad

    (Whitehead Institute for Biomedical Research
    Massachusetts Institute of Technology)

  • Matthew D. Edwards

    (Massachusetts Institute of Technology)

  • Lachlan Mcintosh

    (Walter and Eliza Hall Institute
    Peter MacCallum Cancer Centre
    University of Melbourne)

  • Anthony T. Papenfuss

    (Walter and Eliza Hall Institute
    The University of Melbourne
    Peter MacCallum Cancer Centre
    University of Melbourne)

  • Ann Emery

    (University of North Carolina at Chapel Hill
    University of North Carolina at Chapel Hill
    University of North Carolina at Chapel Hill)

  • Ronald Swanstrom

    (University of North Carolina at Chapel Hill
    University of North Carolina at Chapel Hill
    University of North Carolina at Chapel Hill)

  • Trinity Zang

    (The Rockefeller University)

  • Tammy C. T. Lan

    (Whitehead Institute for Biomedical Research)

  • Paul Bieniasz

    (The Rockefeller University
    The Rockefeller University)

  • Daniel R. Kuritzkes

    (Brigham and Women’s Hospital
    Harvard Medical School)

  • Athe Tsibris

    (Brigham and Women’s Hospital
    Harvard Medical School)

  • Silvi Rouskin

    (Whitehead Institute for Biomedical Research)

Abstract

Human immunodeficiency virus 1 (HIV-1) is a retrovirus with a ten-kilobase single-stranded RNA genome. HIV-1 must express all of its gene products from a single primary transcript, which undergoes alternative splicing to produce diverse protein products that include structural proteins and regulatory factors1,2. Despite the critical role of alternative splicing, the mechanisms that drive the choice of splice site are poorly understood. Synonymous RNA mutations that lead to severe defects in splicing and viral replication indicate the presence of unknown cis-regulatory elements3. Here we use dimethyl sulfate mutational profiling with sequencing (DMS-MaPseq) to investigate the structure of HIV-1 RNA in cells, and develop an algorithm that we name ‘detection of RNA folding ensembles using expectation–maximization’ (DREEM), which reveals the alternative conformations that are assumed by the same RNA sequence. Contrary to previous models that have analysed population averages4, our results reveal heterogeneous regions of RNA structure across the entire HIV-1 genome. In addition to confirming that in vitro characterized5 alternative structures for the HIV-1 Rev responsive element also exist in cells, we discover alternative conformations at critical splice sites that influence the ratio of transcript isoforms. Our simultaneous measurement of splicing and intracellular RNA structure provides evidence for the long-standing hypothesis6–8 that heterogeneity in RNA conformation regulates splice-site use and viral gene expression.

Suggested Citation

  • Phillip J. Tomezsko & Vincent D. A. Corbin & Paromita Gupta & Harish Swaminathan & Margalit Glasgow & Sitara Persad & Matthew D. Edwards & Lachlan Mcintosh & Anthony T. Papenfuss & Ann Emery & Ronald , 2020. "Determination of RNA structural diversity and its role in HIV-1 RNA splicing," Nature, Nature, vol. 582(7812), pages 438-442, June.
  • Handle: RePEc:nat:nature:v:582:y:2020:i:7812:d:10.1038_s41586-020-2253-5
    DOI: 10.1038/s41586-020-2253-5
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    Cited by:

    1. Agnieszka Lipieta & Elżbieta Pliś, 2022. "Diversity and mechanisms of economic evolution," Journal of Evolutionary Economics, Springer, vol. 32(4), pages 1265-1286, September.

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