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The level of protein in the maternal murine diet modulates the facial appearance of the offspring via mTORC1 signaling

Author

Listed:
  • Meng Xie

    (Karolinska Institutet
    Karolinska Institute
    Peking University)

  • Markéta Kaiser

    (Brno University of Technology)

  • Yaakov Gershtein

    (Medical University of Vienna)

  • Daniela Schnyder

    (Karolinska Institutet
    Sahlgrenska Academy at University of Gothenburg)

  • Ruslan Deviatiiarov

    (Kazan Federal University
    Endocrinology Research Center
    Life Improvement by Future Technologies (LIFT) Center
    Juntendo University)

  • Guzel Gazizova

    (Kazan Federal University)

  • Elena Shagimardanova

    (Kazan Federal University
    Life Improvement by Future Technologies (LIFT) Center)

  • Tomáš Zikmund

    (Brno University of Technology)

  • Greet Kerckhofs

    (Biomechanics Lab, Institute of Mechanics, Materials, and Civil Engineering (iMMC), UCLouvain
    Pole of Morphology, Institute of Experimental and Clinical Research (IREC), UCLouvain
    KU Leuven
    Prometheus, Division for Skeletal Tissue Engineering, KU Leuven)

  • Evgeny Ivashkin

    (A.N. Severtsov Institute of Ecology and Evolution, Russian Academy of Sciences
    Russian Academy of Sciences)

  • Dominyka Batkovskyte

    (Karolinska Institutet)

  • Phillip T. Newton

    (Karolinska Institutet
    Karolinska Institutet
    Astrid Lindgren Children’s hospital)

  • Olov Andersson

    (Karolinska Institutet)

  • Kaj Fried

    (Karolinska Institutet)

  • Oleg Gusev

    (Kazan Federal University
    Endocrinology Research Center
    Life Improvement by Future Technologies (LIFT) Center
    Juntendo University)

  • Hugo Zeberg

    (Karolinska Institutet)

  • Jozef Kaiser

    (Brno University of Technology)

  • Igor Adameyko

    (Karolinska Institutet
    Medical University of Vienna)

  • Andrei S. Chagin

    (Karolinska Institutet
    Sahlgrenska Academy at University of Gothenburg)

Abstract

The development of craniofacial skeletal structures is fascinatingly complex and elucidation of the underlying mechanisms will not only provide novel scientific insights, but also help develop more effective clinical approaches to the treatment and/or prevention of the numerous congenital craniofacial malformations. To this end, we performed a genome-wide analysis of RNA transcription from non-coding regulatory elements by CAGE-sequencing of the facial mesenchyme of human embryos and cross-checked the active enhancers thus identified against genes, identified by GWAS for the normal range human facial appearance. Among the identified active cis-enhancers, several belonged to the components of the PI3/AKT/mTORC1/autophagy pathway. To assess the functional role of this pathway, we manipulated it both genetically and pharmacologically in mice and zebrafish. These experiments revealed that mTORC1 signaling modulates craniofacial shaping at the stage of skeletal mesenchymal condensations, with subsequent fine-tuning during clonal intercalation. This ability of mTORC1 pathway to modulate facial shaping, along with its evolutionary conservation and ability to sense external stimuli, in particular dietary amino acids, indicate that the mTORC1 pathway may play a role in facial phenotypic plasticity. Indeed, the level of protein in the diet of pregnant female mice influenced the activity of mTORC1 in fetal craniofacial structures and altered the size of skeletogenic clones, thus exerting an impact on the local geometry and craniofacial shaping. Overall, our findings indicate that the mTORC1 signaling pathway is involved in the effect of environmental conditions on the shaping of craniofacial structures.

Suggested Citation

  • Meng Xie & Markéta Kaiser & Yaakov Gershtein & Daniela Schnyder & Ruslan Deviatiiarov & Guzel Gazizova & Elena Shagimardanova & Tomáš Zikmund & Greet Kerckhofs & Evgeny Ivashkin & Dominyka Batkovskyte, 2024. "The level of protein in the maternal murine diet modulates the facial appearance of the offspring via mTORC1 signaling," Nature Communications, Nature, vol. 15(1), pages 1-15, December.
  • Handle: RePEc:nat:natcom:v:15:y:2024:i:1:d:10.1038_s41467-024-46030-3
    DOI: 10.1038/s41467-024-46030-3
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