Adrienne L Romer1, Maxwell L Elliott1, Annchen R Knodt1, Maria L Sison1, David Ireland1, Renate Houts1, Sandhya Ramrakha1, Richie Poulton1, Ross Keenan1, Tracy R Melzer1, Terrie E Moffitt1, Avshalom Caspi1, Ahmad R Hariri1. 1. Laboratory of NeuroGenetics (Romer, Elliott, Knodt, Sison, Hariri), Department of Psychology and Neuroscience (Romer, Knodt, Houts, Moffitt, Caspi, Hariri), Department of Psychiatry and Behavioral Sciences (Moffitt, Caspi), and Center for Genomic and Computational Biology (Moffitt, Caspi), Duke University, Durham, N.C.; Dunedin Multidisciplinary Health and Development Research Unit, Department of Psychology, University of Otago, Dunedin, New Zealand (Ireland, Ramrakha, Poulton); Christchurch Radiology Group, Christchurch, New Zealand (Keenan); Department of Medicine, University of Otago, Christchurch (Melzer); New Zealand Brain Research Institute, Christchurch (Melzer); Social, Genetic, and Developmental Psychiatry Research Center, Institute of Psychiatry, Psychology, and Neuroscience, King's College London (Moffitt, Caspi); and McLean Hospital/Harvard Medical School, Belmont, Mass. (Romer).
Abstract
OBJECTIVE: Neuroimaging research has revealed that structural brain alterations are common across broad diagnostic families of disorders rather than specific to a single psychiatric disorder. Such overlap in the structural brain correlates of mental disorders mirrors already well-documented phenotypic comorbidity of psychiatric symptoms and diagnoses, which can be indexed by a general psychopathology or p factor. The authors hypothesized that if general psychopathology drives the convergence of structural alterations common across disorders, then 1) there should be few associations unique to any one diagnostic family of disorders, and 2) associations with the p factor should overlap with those for the broader diagnostic families. METHODS: Analyses were conducted on structural MRI and psychopathology data collected from 861 members of the population-representative Dunedin Multidisciplinary Health and Development Study at age 45. RESULTS: Study members with high scores across three broad diagnostic families of disorders (externalizing, internalizing, thought disorder) exhibited highly overlapping patterns of reduced global and widely distributed parcel-wise neocortical thickness. Study members with high p factor scores exhibited patterns of reduced global and parcel-wise neocortical thickness nearly identical to those associated with the three broad diagnostic families. CONCLUSIONS: A pattern of pervasively reduced neocortical thickness appears to be common across all forms of mental disorders and may represent a transdiagnostic feature of general psychopathology. As has been documented with regard to symptoms and diagnoses, the underlying brain structural correlates of mental disorders may not exhibit specificity, and the continued pursuit of such specific correlates may limit progress toward more effective strategies for etiological understanding, prevention, and intervention.
OBJECTIVE: Neuroimaging research has revealed that structural brain alterations are common across broad diagnostic families of disorders rather than specific to a single psychiatric disorder. Such overlap in the structural brain correlates of mental disorders mirrors already well-documented phenotypic comorbidity of psychiatric symptoms and diagnoses, which can be indexed by a general psychopathology or p factor. The authors hypothesized that if general psychopathology drives the convergence of structural alterations common across disorders, then 1) there should be few associations unique to any one diagnostic family of disorders, and 2) associations with the p factor should overlap with those for the broader diagnostic families. METHODS: Analyses were conducted on structural MRI and psychopathology data collected from 861 members of the population-representative Dunedin Multidisciplinary Health and Development Study at age 45. RESULTS: Study members with high scores across three broad diagnostic families of disorders (externalizing, internalizing, thought disorder) exhibited highly overlapping patterns of reduced global and widely distributed parcel-wise neocortical thickness. Study members with high p factor scores exhibited patterns of reduced global and parcel-wise neocortical thickness nearly identical to those associated with the three broad diagnostic families. CONCLUSIONS: A pattern of pervasively reduced neocortical thickness appears to be common across all forms of mental disorders and may represent a transdiagnostic feature of general psychopathology. As has been documented with regard to symptoms and diagnoses, the underlying brain structural correlates of mental disorders may not exhibit specificity, and the continued pursuit of such specific correlates may limit progress toward more effective strategies for etiological understanding, prevention, and intervention.
Entities:
Keywords:
Cortical Thickness; General Psychopathology; Neuroimaging; Transdiagnostic; p Factor
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