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Monoterpenoid aryl hydrocarbon receptor allosteric antagonists protect against ultraviolet skin damage in female mice

Author

Listed:
  • Karolína Ondrová

    (Palacký University)

  • Iveta Zůvalová

    (Palacký University)

  • Barbora Vyhlídalová

    (Palacký University)

  • Kristýna Krasulová

    (Palacký University)

  • Eva Miková

    (Palacký University)

  • Radim Vrzal

    (Palacký University)

  • Petr Nádvorník

    (Palacký University)

  • Binod Nepal

    (Drexel University College of Medicine)

  • Sandhya Kortagere

    (Drexel University College of Medicine)

  • Martina Kopečná

    (Palacký University)

  • David Kopečný

    (Palacký University)

  • Marek Šebela

    (Palacký University)

  • Fraydoon Rastinejad

    (Target Discovery Institute Nuffield Department of Medicine Research Building Brasenose College University of Oxford)

  • Hua Pu

    (Target Discovery Institute Nuffield Department of Medicine Research Building Brasenose College University of Oxford)

  • Miroslav Soural

    (Palacký University)

  • Katharina Maria Rolfes

    (IUF-Leibniz-Research Institute for Environmental Medicine)

  • Thomas Haarmann-Stemmann

    (IUF-Leibniz-Research Institute for Environmental Medicine)

  • Hao Li

    (Albert Einstein College of Medicine)

  • Sridhar Mani

    (Albert Einstein College of Medicine)

  • Zdeněk Dvořák

    (Palacký University)

Abstract

The human aryl hydrocarbon receptor (AhR) is a ligand-activated transcription factor that is a pivotal regulator of human physiology and pathophysiology. Allosteric inhibition of AhR was previously thought to be untenable. Here, we identify carvones as noncompetitive, insurmountable antagonists of AhR and characterize the structural and functional consequences of their binding. Carvones do not displace radiolabeled ligands from binding to AhR but instead bind allosterically within the bHLH/PAS-A region of AhR. Carvones do not influence the translocation of ligand-activated AhR into the nucleus but inhibit the heterodimerization of AhR with its canonical partner ARNT and subsequent binding of AhR to the promoter of CYP1A1. As a proof of concept, we demonstrate physiologically relevant Ahr-antagonism by carvones in vivo in female mice. These substances establish the molecular basis for selective targeting of AhR regardless of the type of ligand(s) present and provide opportunities for the treatment of disease processes modified by AhR.

Suggested Citation

  • Karolína Ondrová & Iveta Zůvalová & Barbora Vyhlídalová & Kristýna Krasulová & Eva Miková & Radim Vrzal & Petr Nádvorník & Binod Nepal & Sandhya Kortagere & Martina Kopečná & David Kopečný & Marek Šeb, 2023. "Monoterpenoid aryl hydrocarbon receptor allosteric antagonists protect against ultraviolet skin damage in female mice," Nature Communications, Nature, vol. 14(1), pages 1-15, December.
  • Handle: RePEc:nat:natcom:v:14:y:2023:i:1:d:10.1038_s41467-023-38478-6
    DOI: 10.1038/s41467-023-38478-6
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    References listed on IDEAS

    as
    1. Jakub Gruszczyk & Loïc Grandvuillemin & Josephine Lai-Kee-Him & Matteo Paloni & Christos G. Savva & Pierre Germain & Marina Grimaldi & Abdelhay Boulahtouf & Hok-Sau Kwong & Julien Bous & Aurélie Ancel, 2022. "Cryo-EM structure of the agonist-bound Hsp90-XAP2-AHR cytosolic complex," Nature Communications, Nature, vol. 13(1), pages 1-13, December.
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    3. Lisa Maier & Mihaela Pruteanu & Michael Kuhn & Georg Zeller & Anja Telzerow & Exene Erin Anderson & Ana Rita Brochado & Keith Conrad Fernandez & Hitomi Dose & Hirotada Mori & Kiran Raosaheb Patil & Pe, 2018. "Extensive impact of non-antibiotic drugs on human gut bacteria," Nature, Nature, vol. 555(7698), pages 623-628, March.
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