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N-terminal acetylation shields proteins from degradation and promotes age-dependent motility and longevity

Author

Listed:
  • Sylvia Varland

    (University of Bergen
    University of Bergen
    University of Toronto)

  • Rui Duarte Silva

    (Universidade do Algarve
    Universidade do Algarve)

  • Ine Kjosås

    (University of Bergen)

  • Alexandra Faustino

    (Universidade do Algarve)

  • Annelies Bogaert

    (VIB-UGent Center for Medical Biotechnology
    Ghent University)

  • Maximilian Billmann

    (University of Minnesota-Twin Cities
    University of Bonn, School of Medicine and University Hospital Bonn)

  • Hadi Boukhatmi

    (Université de Rennes 1, CNRS, UMR6290)

  • Barbara Kellen

    (Universidade do Algarve)

  • Michael Costanzo

    (University of Toronto)

  • Adrian Drazic

    (University of Bergen)

  • Camilla Osberg

    (University of Bergen)

  • Katherine Chan

    (University of Toronto)

  • Xiang Zhang

    (University of Minnesota-Twin Cities)

  • Amy Hin Yan Tong

    (University of Toronto)

  • Simonetta Andreazza

    (University of Cambridge)

  • Juliette J. Lee

    (University of Cambridge)

  • Lyudmila Nedyalkova

    (University of Toronto)

  • Matej Ušaj

    (University of Toronto)

  • Alexander J. Whitworth

    (University of Cambridge)

  • Brenda J. Andrews

    (University of Toronto
    University of Toronto)

  • Jason Moffat

    (University of Toronto
    University of Toronto
    The Hospital for Sick Children)

  • Chad L. Myers

    (University of Minnesota-Twin Cities
    University of Minnesota-Twin Cities)

  • Kris Gevaert

    (VIB-UGent Center for Medical Biotechnology
    Ghent University)

  • Charles Boone

    (University of Toronto
    University of Toronto
    RIKEN Centre for Sustainable Resource Science, Wako)

  • Rui Gonçalo Martinho

    (Universidade do Algarve
    Universidade de Aveiro
    Universidade de Aveiro)

  • Thomas Arnesen

    (University of Bergen
    University of Bergen
    Haukeland University Hospital)

Abstract

Most eukaryotic proteins are N-terminally acetylated, but the functional impact on a global scale has remained obscure. Using genome-wide CRISPR knockout screens in human cells, we reveal a strong genetic dependency between a major N-terminal acetyltransferase and specific ubiquitin ligases. Biochemical analyses uncover that both the ubiquitin ligase complex UBR4-KCMF1 and the acetyltransferase NatC recognize proteins bearing an unacetylated N-terminal methionine followed by a hydrophobic residue. NatC KO-induced protein degradation and phenotypes are reversed by UBR knockdown, demonstrating the central cellular role of this interplay. We reveal that loss of Drosophila NatC is associated with male sterility, reduced longevity, and age-dependent loss of motility due to developmental muscle defects. Remarkably, muscle-specific overexpression of UbcE2M, one of the proteins targeted for NatC KO-mediated degradation, suppresses defects of NatC deletion. In conclusion, NatC-mediated N-terminal acetylation acts as a protective mechanism against protein degradation, which is relevant for increased longevity and motility.

Suggested Citation

  • Sylvia Varland & Rui Duarte Silva & Ine Kjosås & Alexandra Faustino & Annelies Bogaert & Maximilian Billmann & Hadi Boukhatmi & Barbara Kellen & Michael Costanzo & Adrian Drazic & Camilla Osberg & Kat, 2023. "N-terminal acetylation shields proteins from degradation and promotes age-dependent motility and longevity," Nature Communications, Nature, vol. 14(1), pages 1-27, December.
  • Handle: RePEc:nat:natcom:v:14:y:2023:i:1:d:10.1038_s41467-023-42342-y
    DOI: 10.1038/s41467-023-42342-y
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    References listed on IDEAS

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    1. Yao Li & Yueling Zhao & Xiaojie Yan & Chen Ye & Sara Weirich & Bing Zhang & Xiaolu Wang & Lili Song & Chenhao Jiang & Albert Jeltsch & Cheng Dong & Wenyi Mi, 2022. "CRL2ZER1/ZYG11B recognizes small N-terminal residues for degradation," Nature Communications, Nature, vol. 13(1), pages 1-11, December.
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