Reproducible Sex Differences in Personalized Functional Network Topography in Youth

  1. Arielle S. Keller
  2. Kevin Y. Sun
  3. Ashley Francisco
  4. Heather Robinson
  5. Emily Beydler
  6. Dani S. Bassett
  7. Matthew Cieslak
  8. Zaixu Cui
  9. Christos Davatzikos
  10. Yong Fan
  11. Margaret Gardner
  12. Rachel Kishton
  13. Sara L. Kornfield
  14. Bart Larsen
  15. Hongming Li
  16. Isabella Linder
  17. Adam Pines
  18. Laura Pritschet
  19. Armin Raznahan
  20. David R. Roalf
  21. Jakob Seidlitz
  22. Golia Shafiei
  23. Russell T. Shinohara
  24. Daniel H. Wolf
  25. Aaron Alexander-Bloch
  26. Theodore D. Satterthwaite
  27. Sheila Shanmugan
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Abstract

Background

A key step towards understanding psychiatric disorders that disproportionately impact female mental health is delineating the emergence of sex-specific patterns of brain organization at the critical transition from childhood to adolescence. Prior work suggests that individual differences in the spatial organization of functional brain networks across the cortex are associated with psychopathology and differ systematically by sex.

Aims

We aimed to evaluate the impact of sex on the spatial organization of person-specific functional brain networks.

Method

We leveraged person-specific atlases of functional brain networks defined using non-negative matrix factorization in a sample of n = 6437 youths from the Adolescent Brain Cognitive Development Study. Across independent discovery and replication samples, we used generalized additive models to uncover associations between sex and the spatial layout (“topography”) of personalized functional networks (PFNs). Next, we trained support vector machines to classify participants’ sex from multivariate patterns of PFN topography. Finally, we leveraged transcriptomic data from the Allen Human Brain Atlas to evaluate spatial correlations between sex differences in PFN topography and gene expression.

Results

Sex differences in PFN topography were greatest in association networks including the fronto-parietal, ventral attention, and default mode networks. Machine learning models trained on participants’ PFNs were able to classify participant sex with high accuracy. Brain regions with the greatest sex differences in PFN topography were enriched in expression of X-linked genes as well as genes expressed in astrocytes and excitatory neurons.

Conclusions

Sex differences in PFN topography are robust, replicate across large-scale samples of youth, and are associated with expression patterns of X-linked genes. These results suggest a potential contributor to the female-biased risk in depressive and anxiety disorders that emerge at the transition from childhood to adolescence.

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  1. Version published to 10.1101/2024.09.26.615061v1 on bioRxiv