PT - JOURNAL ARTICLE AU - van der Wijk, Gwen AU - Zamyadi, Mojdeh AU - Bray, Signe AU - Hassel, Stefanie AU - Arnott, Stephen R. AU - Frey, Benicio N. AU - Kennedy, Sidney H. AU - Davis, Andrew D. AU - Hall, Geoffrey B. AU - Lam, Raymond W. AU - Milev, Roumen AU - Müller, Daniel J. AU - Parikh, Sagar AU - Soares, Claudio AU - Macqueen, Glenda M. AU - Strother, Stephen C. AU - Protzner, Andrea B. TI - Large Individual Differences in Functional Connectivity in the Context of Major Depression and Antidepressant Pharmacotherapy AID - 10.1523/ENEURO.0286-23.2024 DP - 2024 Jun 03 TA - eneuro PG - ENEURO.0286-23.2024 4099 - http://www.eneuro.org/content/early/2024/05/25/ENEURO.0286-23.2024.short 4100 - http://www.eneuro.org/content/early/2024/05/25/ENEURO.0286-23.2024.full AB - Clinical studies of major depression (MD) generally focus on group effects, yet inter-individual differences in brain function are increasingly recognised as important and may even impact effect sizes related to group effects. Here, we examine the magnitude of individual differences in relation to group differences that are commonly investigated (e.g., related to MD diagnosis and treatment response). Functional MRI data from 107 participants (63 female, 44 male) were collected at baseline, 2 and 8 weeks during which patients received pharmacotherapy (escitalopram, N=68), and controls (N=39) received no intervention. The unique contributions of different sources of variation were examined by calculating how much variance in functional connectivity was shared across all participants and sessions, within/across groups (patients vs controls, responders vs non-responders, female vs male participants), recording sessions and individuals. Individual differences and common connectivity across groups, sessions and participants contributed most to the explained variance (>95% across analyses). Group differences related to MD diagnosis, treatment response and biological sex made significant but small contributions (0.3-1.2%). High individual variation was present in cognitive control and attention areas, while low individual variation characterized primary sensorimotor regions. Group differences were much smaller than individual differences in the context of MD and its treatment. These results could be linked to the variable findings and difficulty translating research on MD to clinical practice. Future research should examine brain features with low and high individual variation in relation to psychiatric symptoms and treatment trajectories to explore the clinical relevance of the individual differences identified here.Significance statement Studies on major depression often investigate differences in brain function between groups (e.g., those with/without a diagnosis) to better understand this prevalent condition. Our study examines such group differences in the context of similarities across and differences between individuals. We found strong common and individually unique features of brain network organization, relative to surprisingly subtle features of diagnosis, treatment success, and sex assigned at birth. From the overall explained variation in brain connectivity, about 50% was shared across everyone, while another 45% was unique to individuals. Only ∼5% could be attributed to group differences. Our results suggest that examining individual differences, and their potential clinical relevance, alongside group differences may bring us closer to improving clinical outcomes for major depression.