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Unique genetic and risk-factor profiles in clusters of major depressive disorder-related multimorbidity trajectories

Author

Listed:
  • Andras Gezsi

    (Budapest University of Technology and Economics)

  • Sandra Auwera

    (University Medicine Greifswald
    Site Rostock/Greifswald)

  • Hannu Mäkinen

    (Finnish Institute for Health and Welfare)

  • Nora Eszlari

    (Semmelweis University
    Semmelweis University)

  • Gabor Hullam

    (Budapest University of Technology and Economics
    Semmelweis University)

  • Tamas Nagy

    (Budapest University of Technology and Economics
    Semmelweis University
    Semmelweis University)

  • Sarah Bonk

    (University Medicine Greifswald)

  • Rubèn González-Colom

    (Universitat de Barcelona)

  • Xenia Gonda

    (Semmelweis University
    Semmelweis University
    Semmelweis University)

  • Linda Garvert

    (University Medicine Greifswald)

  • Teemu Paajanen

    (Finnish Institute for Health and Welfare)

  • Zsofia Gal

    (Semmelweis University
    Semmelweis University)

  • Kevin Kirchner

    (University Medicine Greifswald)

  • Andras Millinghoffer

    (Abiomics Europe Ltd.)

  • Carsten O. Schmidt

    (University Medicine Greifswald)

  • Bence Bolgar

    (Budapest University of Technology and Economics)

  • Josep Roca

    (Universitat de Barcelona)

  • Isaac Cano

    (Universitat de Barcelona)

  • Mikko Kuokkanen

    (Finnish Institute for Health and Welfare
    School of Medicine at University of Texas Rio Grande Valley
    University of Helsinki)

  • Peter Antal

    (Budapest University of Technology and Economics)

  • Gabriella Juhasz

    (Semmelweis University
    Semmelweis University)

Abstract

The heterogeneity and complexity of symptom presentation, comorbidities and genetic factors pose challenges to the identification of biological mechanisms underlying complex diseases. Current approaches used to identify biological subtypes of major depressive disorder (MDD) mainly focus on clinical characteristics that cannot be linked to specific biological models. Here, we examined multimorbidities to identify MDD subtypes with distinct genetic and non-genetic factors. We leveraged dynamic Bayesian network approaches to determine a minimal set of multimorbidities relevant to MDD and identified seven clusters of disease-burden trajectories throughout the lifespan among 1.2 million participants from cohorts in the UK, Finland, and Spain. The clusters had clear protective- and risk-factor profiles as well as age-specific clinical courses mainly driven by inflammatory processes, and a comprehensive map of heritability and genetic correlations among these clusters was revealed. Our results can guide the development of personalized treatments for MDD based on the unique genetic, clinical and non-genetic risk-factor profiles of patients.

Suggested Citation

  • Andras Gezsi & Sandra Auwera & Hannu Mäkinen & Nora Eszlari & Gabor Hullam & Tamas Nagy & Sarah Bonk & Rubèn González-Colom & Xenia Gonda & Linda Garvert & Teemu Paajanen & Zsofia Gal & Kevin Kirchner, 2024. "Unique genetic and risk-factor profiles in clusters of major depressive disorder-related multimorbidity trajectories," Nature Communications, Nature, vol. 15(1), pages 1-18, December.
  • Handle: RePEc:nat:natcom:v:15:y:2024:i:1:d:10.1038_s41467-024-51467-7
    DOI: 10.1038/s41467-024-51467-7
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    References listed on IDEAS

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