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Plasticity of the mammalian integrated stress response

Author

Listed:
  • Chien-Wen Chen

    (Case Western Reserve University)

  • David Papadopoli

    (Sir Mortimer B. Davis-Jewish General Hospital
    McGill University)

  • Krzysztof J. Szkop

    (Science of Life Laboratory)

  • Bo-Jhih Guan

    (Case Western Reserve University)

  • Mohammed Alzahrani

    (Case Western Reserve University
    King Saud bin Abdulaziz University for Health Sciences
    King Abdullah International Medical Research Center)

  • Jing Wu

    (Case Western Reserve University)

  • Raul Jobava

    (Case Western Reserve University
    Yale University)

  • Mais M. Asraf

    (Case Western Reserve University)

  • Dawid Krokowski

    (Maria Curie-Skłodowska University)

  • Anastasios Vourekas

    (Louisiana State University)

  • William C. Merrick

    (Case Western Reserve University)

  • Anton A. Komar

    (Case Western Reserve University
    Cleveland State University)

  • Antonis E. Koromilas

    (Sir Mortimer B. Davis-Jewish General Hospital
    McGill University
    McGill University)

  • Myriam Gorospe

    (NIH)

  • Matthew J. Payea

    (NIH)

  • Fangfang Wang

    (Case Western Reserve University)

  • Benjamin L. L. Clayton

    (Case Western Reserve University
    School of Medicine)

  • Paul J. Tesar

    (Case Western Reserve University
    School of Medicine)

  • Ashleigh Schaffer

    (Case Western Reserve University)

  • Alexander Miron

    (Case Western Reserve University)

  • Ilya Bederman

    (Case Western Reserve University)

  • Eckhard Jankowsky

    (Case Western Reserve University)

  • Christine Vogel

    (New York University)

  • Leoš Shivaya Valášek

    (Institute of Microbiology of the Czech Academy of Sciences)

  • Jonathan D. Dinman

    (University of Maryland
    University of Maryland)

  • Youwei Zhang

    (Case Western Reserve University)

  • Boaz Tirosh

    (Case Western Reserve University)

  • Ola Larsson

    (Science of Life Laboratory)

  • Ivan Topisirovic

    (Sir Mortimer B. Davis-Jewish General Hospital
    McGill University
    McGill University
    McGill University)

  • Maria Hatzoglou

    (Case Western Reserve University)

Abstract

An increased level of phosphorylation of eukaryotic translation initiation factor 2 subunit-α (eIF2α, encoded by EIF2S1; eIF2α-p) coupled with decreased guanine nucleotide exchange activity of eIF2B is a hallmark of the ‘canonical’ integrated stress response (c-ISR)1. It is unclear whether impaired eIF2B activity in human diseases including leukodystrophies2, which occurs in the absence of eIF2α-p induction, is synonymous with the c-ISR. Here we describe a mechanism triggered by decreased eIF2B activity, distinct from the c-ISR, which we term the split ISR (s-ISR). The s-ISR is characterized by translational and transcriptional programs that are different from those observed in the c-ISR. Opposite to the c-ISR, the s-ISR requires eIF4E-dependent translation of the upstream open reading frame 1 and subsequent stabilization of ATF4 mRNA. This is followed by altered expression of a subset of metabolic genes (for example, PCK2), resulting in metabolic rewiring required to maintain cellular bioenergetics when eIF2B activity is attenuated. Overall, these data demonstrate a plasticity of the mammalian ISR, whereby the loss of eIF2B activity in the absence of eIF2α-p induction activates the eIF4E–ATF4–PCK2 axis to maintain energy homeostasis.

Suggested Citation

  • Chien-Wen Chen & David Papadopoli & Krzysztof J. Szkop & Bo-Jhih Guan & Mohammed Alzahrani & Jing Wu & Raul Jobava & Mais M. Asraf & Dawid Krokowski & Anastasios Vourekas & William C. Merrick & Anton , 2025. "Plasticity of the mammalian integrated stress response," Nature, Nature, vol. 641(8065), pages 1319-1328, May.
  • Handle: RePEc:nat:nature:v:641:y:2025:i:8065:d:10.1038_s41586-025-08794-6
    DOI: 10.1038/s41586-025-08794-6
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