Genome-wide association study of adolescent-onset depression
Abstract
Adolescent depression is a heritable psychiatric condition with rising global prevalence and severe long-term outcomes, yet its biological underpinnings remain poorly understood. We conducted the first genome-wide association study of adolescent-onset depression, comprising 102,428 cases (diagnosis or clinical symptom thresholds) and 286,911 controls, including diverse ancestries.
Cross-ancestry meta-analysis identified 52 independent variants across 17 loci; European-only analysis found 61 variants at 29 loci, with a SNP-based heritability of 9.8%. Comparative analyses revealed two genes unique to adolescent-onset versus lifetime depression, enriched in neuronal subtypes, and two genes as potential drug repurposing targets.
Polygenic scores were associated with adolescent-onset depression across ancestries, persistent depression trajectories, more severe outcomes, as well as reduced cortical volume, surface area and white matter integrity. Genetic correlation and Mendelian randomisation analyses support shared genetic liability and causal links with early puberty and modifiable health and behavioural risk factors.
These findings uncover novel genetic loci and refine biological pathways underlying adolescent-onset depression, revealing age-specific mechanisms and early intervention opportunities.
Web | PDF | Preprint: MedRxiv | Open Access
Poppy Z Grimes, Brittany L Mitchell, Katherine N Thompson, Qingkun Deng, Xueyi Shen, Jareth C Wolfe, Jodi T Thomas, Robyn E Wootton, Daniel E Adkins, Saranya Arirangan, Elham Assary, Chris Chatzinakos, Charlotte A Dennison, Swathi Hassan Gangaraju, Andreas Jangmo, Yeongmi Jeong, Siim Kurvits, Qingqin S Li, Ehsan Motazedi, Joonas Naamanka, Thuy-Dung Nguyen, Ilja M Nolte, Vanessa K Ota, Joëlle A Pasman, Mina Shahisavandi, Amy Shakeshaft, John R Shorter, Chloe Slaney, Martin Tesli, Carol A Wang, Uxue Zubizarreta-Arruti, PGC MDD Working Group, GLAD+, NIHR BioResource, Silvia Alemany, Ole A Andreassen, Helga Ask, Sintia I Belangero, Rosa Bosch, Gerome Breen, Rodrigo A Bressan, Alfonso Buil, Enda M Byrne, Miquel Casas, William E Copeland, Thalia C Eley, Laurie J Hannigan, Catharina A Hartman, Alexandra Havdahl, Ian B Hickie, Golam M Khandaker, Kelli Lehto, Hermine Maes, Nicholas G Martin, Alexander Neumann, Albertine J Oldehinkel, Pedro M Pan, Hong Pan, Craig E Pennell, Roseann E Peterson, Alina Rodriguez, Giovanni A Salum, Tanja GM Vrijkotte, Robbee Wedow, Andrew JO Whitehouse, Anita Thapar, Henrik Larsson, Christel M Middeldorp, Andrew McIntosh, Mark J Adams, Yi Lu, Heather C Whalley, Alex SF Kwong
Abstract
Adolescent depression is a heritable psychiatric condition with rising global prevalence and severe long-term outcomes, yet its biological underpinnings remain poorly understood. We conducted the first genome-wide association study of adolescent-onset depression, comprising 102,428 cases (diagnosis or clinical symptom thresholds) and 286,911 controls, including diverse ancestries.
Cross-ancestry meta-analysis identified 52 independent variants across 17 loci; European-only analysis found 61 variants at 29 loci, with a SNP-based heritability of 9.8%. Comparative analyses revealed two genes unique to adolescent-onset versus lifetime depression, enriched in neuronal subtypes, and two genes as potential drug repurposing targets.
Polygenic scores were associated with adolescent-onset depression across ancestries, persistent depression trajectories, more severe outcomes, as well as reduced cortical volume, surface area and white matter integrity. Genetic correlation and Mendelian randomisation analyses support shared genetic liability and causal links with early puberty and modifiable health and behavioural risk factors.
These findings uncover novel genetic loci and refine biological pathways underlying adolescent-onset depression, revealing age-specific mechanisms and early intervention opportunities.
Web | PDF | Preprint: MedRxiv | Open Access