Modeling brain sex in the limbic system as phenotype for female-prevalent mental disorders

Gloria Matte Bon; Dominik Kraft; Erika Comasco; Birgit Derntl; Tobias Kaufmann

doi:10.1186/s13293-024-00615-1

Biology of Sex Differences (May 2024)

Modeling brain sex in the limbic system as phenotype for female-prevalent mental disorders

Gloria Matte Bon,
Dominik Kraft,
Erika Comasco,
Birgit Derntl,
Tobias Kaufmann

Affiliations

Gloria Matte Bon: Department of Psychiatry and Psychotherapy, Tübingen Center for Mental Health, University of Tübingen
Dominik Kraft: Department of Psychiatry and Psychotherapy, Tübingen Center for Mental Health, University of Tübingen
Erika Comasco: Department of Women’s and Children’s Health, Science for Life Laboratory, Uppsala University
Birgit Derntl: Department of Psychiatry and Psychotherapy, Tübingen Center for Mental Health, University of Tübingen
Tobias Kaufmann: Department of Psychiatry and Psychotherapy, Tübingen Center for Mental Health, University of Tübingen

DOI: https://doi.org/10.1186/s13293-024-00615-1
Journal volume & issue: Vol. 15, no. 1
pp. 1 – 15

Abstract

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Abstract Background Sex differences exist in the prevalence and clinical manifestation of several mental disorders, suggesting that sex-specific brain phenotypes may play key roles. Previous research used machine learning models to classify sex from imaging data of the whole brain and studied the association of class probabilities with mental health, potentially overlooking regional specific characteristics. Methods We here investigated if a regionally constrained model of brain volumetric imaging data may provide estimates that are more sensitive to mental health than whole brain-based estimates. Given its known role in emotional processing and mood disorders, we focused on the limbic system. Using two different cohorts of healthy subjects, the Human Connectome Project and the Queensland Twin IMaging, we investigated sex differences and heritability of brain volumes of limbic structures compared to non-limbic structures, and subsequently applied regionally constrained machine learning models trained solely on limbic or non-limbic features. To investigate the biological underpinnings of such models, we assessed the heritability of the obtained sex class probability estimates, and we investigated the association with major depression diagnosis in an independent clinical sample. All analyses were performed both with and without controlling for estimated total intracranial volume (eTIV). Results Limbic structures show greater sex differences and are more heritable compared to non-limbic structures in both analyses, with and without eTIV control. Consequently, machine learning models performed well at classifying sex based solely on limbic structures and achieved performance as high as those on non-limbic or whole brain data, despite the much smaller number of features in the limbic system. The resulting class probabilities were heritable, suggesting potentially meaningful underlying biological information. Applied to an independent population with major depressive disorder, we found that depression is associated with male–female class probabilities, with largest effects obtained using the limbic model. This association was significant for models not controlling for eTIV whereas in those controlling for eTIV the associations did not pass significance correction. Conclusions Overall, our results highlight the potential utility of regionally constrained models of brain sex to better understand the link between sex differences in the brain and mental disorders.

Published in Biology of Sex Differences

ISSN: 2042-6410 (Online)
Publisher: BMC
Country of publisher: United Kingdom
LCC subjects: Medicine; Science: Physiology
Website: http://bsd.biomedcentral.com

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Abstract

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