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Scleral PERK and ATF6 as targets of myopic axial elongation of mouse eyes

Author

Listed:
  • Shin-ichi Ikeda

    (Keio University School of Medicine
    Keio University School of Medicine)

  • Toshihide Kurihara

    (Keio University School of Medicine
    Keio University School of Medicine)

  • Xiaoyan Jiang

    (Keio University School of Medicine
    Keio University School of Medicine)

  • Yukihiro Miwa

    (Keio University School of Medicine
    Keio University School of Medicine)

  • Deokho Lee

    (Keio University School of Medicine
    Keio University School of Medicine)

  • Naho Serizawa

    (Keio University School of Medicine
    Keio University School of Medicine)

  • Heonuk Jeong

    (Keio University School of Medicine
    Keio University School of Medicine)

  • Kiwako Mori

    (Keio University School of Medicine
    Keio University School of Medicine)

  • Yusaku Katada

    (Keio University School of Medicine
    Keio University School of Medicine)

  • Hiromitsu Kunimi

    (Keio University School of Medicine
    Keio University School of Medicine)

  • Nobuhiro Ozawa

    (Keio University School of Medicine
    Keio University School of Medicine)

  • Chiho Shoda

    (Keio University School of Medicine
    Keio University School of Medicine)

  • Mari Ibuki

    (Keio University School of Medicine
    Keio University School of Medicine)

  • Kazuno Negishi

    (Keio University School of Medicine)

  • Hidemasa Torii

    (Keio University School of Medicine
    Keio University School of Medicine)

  • Kazuo Tsubota

    (Keio University School of Medicine
    Tsubota Laboratory, Inc.)

Abstract

Axial length is the primary determinant of eye size, and it is elongated in myopia. However, the underlying mechanism of the onset and progression of axial elongation remain unclear. Here, we show that endoplasmic reticulum (ER) stress in sclera is an essential regulator of axial elongation in myopia development through activation of both PERK and ATF6 axis followed by scleral collagen remodeling. Mice with lens-induced myopia (LIM) showed ER stress in sclera. Pharmacological interventions for ER stress could induce or inhibit myopia progression. LIM activated all IRE1, PERK and ATF6 axis, and pharmacological inhibition of both PERK and ATF6 suppressed myopia progression, which was confirmed by knocking down above two genes via CRISPR/Cas9 system. LIM dramatically changed the expression of scleral collagen genes responsible for ER stress. Furthermore, collagen fiber thinning and expression of dysregulated collagens in LIM were ameliorated by 4-PBA administration. We demonstrate that scleral ER stress and PERK/ATF6 pathway controls axial elongation during the myopia development in vivo model and 4-PBA eye drop is promising drug for myopia suppression/treatment.

Suggested Citation

  • Shin-ichi Ikeda & Toshihide Kurihara & Xiaoyan Jiang & Yukihiro Miwa & Deokho Lee & Naho Serizawa & Heonuk Jeong & Kiwako Mori & Yusaku Katada & Hiromitsu Kunimi & Nobuhiro Ozawa & Chiho Shoda & Mari , 2022. "Scleral PERK and ATF6 as targets of myopic axial elongation of mouse eyes," Nature Communications, Nature, vol. 13(1), pages 1-14, December.
  • Handle: RePEc:nat:natcom:v:13:y:2022:i:1:d:10.1038_s41467-022-33605-1
    DOI: 10.1038/s41467-022-33605-1
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    References listed on IDEAS

    as
    1. Elie Dolgin, 2015. "The myopia boom," Nature, Nature, vol. 519(7543), pages 276-278, March.
    2. Erik A. Blackwood & Khalid Azizi & Donna J. Thuerauf & Ryan J. Paxman & Lars Plate & Jeffery W. Kelly & R. Luke Wiseman & Christopher C. Glembotski, 2019. "Pharmacologic ATF6 activation confers global protection in widespread disease models by reprograming cellular proteostasis," Nature Communications, Nature, vol. 10(1), pages 1-16, December.
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