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Engineered tRNAs suppress nonsense mutations in cells and in vivo

Author

Listed:
  • Suki Albers

    (University of Hamburg)

  • Elizabeth C. Allen

    (Arcturus Therapeutics)

  • Nikhil Bharti

    (University of Hamburg)

  • Marcos Davyt

    (University of Hamburg)

  • Disha Joshi

    (Emory University
    Children’s Healthcare of Atlanta)

  • Carlos G. Perez-Garcia

    (Arcturus Therapeutics)

  • Leonardo Santos

    (University of Hamburg)

  • Rajesh Mukthavaram

    (Arcturus Therapeutics)

  • Miguel Angel Delgado-Toscano

    (University of Hamburg)

  • Brandon Molina

    (Arcturus Therapeutics)

  • Kristen Kuakini

    (Arcturus Therapeutics)

  • Maher Alayyoubi

    (Arcturus Therapeutics)

  • Kyoung-Joo Jenny Park

    (Arcturus Therapeutics)

  • Grishma Acharya

    (Arcturus Therapeutics)

  • Jose A. Gonzalez

    (Arcturus Therapeutics)

  • Amit Sagi

    (Arcturus Therapeutics)

  • Susan E. Birket

    (University of Alabama at Birmingham)

  • Guillermo J. Tearney

    (Wellman Center for Photomedicine, Massachusetts General Hospital
    Harvard-MIT Health Sciences and Technology)

  • Steven M. Rowe

    (University of Alabama at Birmingham)

  • Candela Manfredi

    (Emory University
    Children’s Healthcare of Atlanta)

  • Jeong S. Hong

    (Emory University
    Children’s Healthcare of Atlanta)

  • Kiyoshi Tachikawa

    (Arcturus Therapeutics)

  • Priya Karmali

    (Arcturus Therapeutics)

  • Daiki Matsuda

    (Arcturus Therapeutics)

  • Eric J. Sorscher

    (Emory University
    Children’s Healthcare of Atlanta)

  • Pad Chivukula

    (Arcturus Therapeutics)

  • Zoya Ignatova

    (University of Hamburg)

Abstract

Nonsense mutations are the underlying cause of approximately 11% of all inherited genetic diseases1. Nonsense mutations convert a sense codon that is decoded by tRNA into a premature termination codon (PTC), resulting in an abrupt termination of translation. One strategy to suppress nonsense mutations is to use natural tRNAs with altered anticodons to base-pair to the newly emerged PTC and promote translation2–7. However, tRNA-based gene therapy has not yielded an optimal combination of clinical efficacy and safety and there is presently no treatment for individuals with nonsense mutations. Here we introduce a strategy based on altering native tRNAs into efficient suppressor tRNAs (sup-tRNAs) by individually fine-tuning their sequence to the physico-chemical properties of the amino acid that they carry. Intravenous and intratracheal lipid nanoparticle (LNP) administration of sup-tRNA in mice restored the production of functional proteins with nonsense mutations. LNP–sup-tRNA formulations caused no discernible readthrough at endogenous native stop codons, as determined by ribosome profiling. At clinically important PTCs in the cystic fibrosis transmembrane conductance regulator gene (CFTR), the sup-tRNAs re-established expression and function in cell systems and patient-derived nasal epithelia and restored airway volume homeostasis. These results provide a framework for the development of tRNA-based therapies with a high molecular safety profile and high efficacy in targeted PTC suppression.

Suggested Citation

  • Suki Albers & Elizabeth C. Allen & Nikhil Bharti & Marcos Davyt & Disha Joshi & Carlos G. Perez-Garcia & Leonardo Santos & Rajesh Mukthavaram & Miguel Angel Delgado-Toscano & Brandon Molina & Kristen , 2023. "Engineered tRNAs suppress nonsense mutations in cells and in vivo," Nature, Nature, vol. 618(7966), pages 842-848, June.
  • Handle: RePEc:nat:nature:v:618:y:2023:i:7966:d:10.1038_s41586-023-06133-1
    DOI: 10.1038/s41586-023-06133-1
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    Cited by:

    1. Nikhil Bharti & Leonardo Santos & Marcos Davyt & Stine Behrmann & Marie Eichholtz & Alejandro Jimenez-Sanchez & Jeong S. Hong & Andras Rab & Eric J. Sorscher & Suki Albers & Zoya Ignatova, 2024. "Translation velocity determines the efficacy of engineered suppressor tRNAs on pathogenic nonsense mutations," Nature Communications, Nature, vol. 15(1), pages 1-10, December.

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