Age-dependent acceleration of structural brain aging in medication-free major depressive disorder linked to neuroanatomical phenotype findings from COORDINATE-MDD consortium
Sharma, B.; Ballester, P. L.; Minuzzi, L.; Xiao, W.; Antoniades, M.; Srinivasan, D.; Erus, G.; Garcia, J.; Fan, Y.; Arnone, D.; Arnott, S.; Chen, T.; Choi, K. S.; Dunlop, K.; Fatt, C. C.; Woodham, R. D.; Godlewska, B.; Hassel, S.; Ho, K.; McIntosh, A. M.; Qin, K.; Rotzinger, S.; Sacchet, M.; Savitz, J.; Shou, H.; Singh, A.; Frokjaer, V.; Ganz, M.; Stolicyn, A.; Strigo, I.; Tosun, D.; Wei, D.; Anderson, I.; Craighead, E.; Deakin, B.; Dunlop, B.; Elliot, R.; Gong, Q.; Gotlib, I.; Harmer, C.; Kennedy, S. H.; Knudsen, G. M.; Mayberg, H.; Paulus, M. P.; Qiu, J.; Trivedi, M.; Whalley, H. C.; Yan, C.
Show abstract
Background: Major depressive disorder (MDD) is associated with altered brain structure and evidence of accelerated brain aging. However, previous studies have been limited by clinical samples with mixed medication status and multiple mood states, modest sample sizes, small percentage of MDD individuals older than 65 years of age, and/or reliance on summary-level data. Methods: Harmonized T1-weighted MRI from MDD (n = 645), all medication-free and in a current depressive episode, and matched healthy controls (n = 645), segmented into 145 regional volumes, from 11 sites in COORDINATE-MDD consortium. Brain age gap (BAG) was estimated using gradient boosting regression with nested cross-validation. Group differences in BAG (and age-corrected BAG [cBAG]) were examined across age strata. Regional contributions were evaluated using Shapley Additive exPlanations. Results: MDD was associated with significantly elevated cBAG compared with healthy controls (mean difference + 2.01 years). Age-stratified analyses showed no differences before mid-30s, with progressively larger gaps thereafter, reaching +6.85 years in MDD aged 55 and older. cBAG differed across neuroanatomical phenotypes associated with differential antidepressant response, cognitive impairment, increased adverse life events, increased self-harm and suicide attempts, and a pro-atherogenic metabolic profile. Key contributing regions included lateral and medial prefrontal regions, middle temporal gyrus, putamen, supplementary motor cortex, central operculum, and cerebellum. Conclusions: Accelerated structural brain aging in MDD is age-dependent and is most pronounced in a neuroanatomical phenotype associated with worse key clinical outcomes. The findings support neuroprogression models of MDD while demonstrating that cBAG is not a uniform feature of MDD and seem to be more strongly expressed in a specifically clinically vulnerable disease phenotype.
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