Abstract
Etiologic insights into psychopathology may be gained by using hypothesis-free methods to identify associations between genetic risk for broad psychopathology and phenotypes measured during adolescence, including both markers of child psychopathology and intermediate phenotypes such as neural structure that may link genetic risk with outcomes. We conducted an exploratory phenome-wide association study (phenotype n=1,271-1,697) of polygenic risk scores (PRS) for broad spectrum psychopathology (i.e., Compulsive, Psychotic, Neurodevelopmental, and Internalizing) in youth of PCA-selected European ancestry (n=5,556; ages 9-13) who completed the baseline and/or two-year follow-up of the ongoing Adolescent Brain Cognitive Development(SM) (ABCD) Study. We found that Neurodevelopmental and Internalizing PRS were significantly associated with phenotypes across multiple domains (Neurodevelopmental: 190 and 214 (147 and 165 after pruning correlated phenotypes at an R(2) of 0.6); Internalizing: 124 and 183 (93 and 131 after pruning) phenotypes at baseline and two-year follow-up, respectively), whereas Compulsive and Psychotic PRS showed zero and two significant associations, respectively, after Bonferroni correction. Compulsive, Psychotic, and Neurodevelopmental PRS were further associated with brain structure metrics, with minimal evidence that brain structure indirectly linked PRS to two-year follow-up outcomes. Genetic variation influencing risk to psychopathology manifests broadly as behaviors, psychopathology symptoms, and related risk factors in middle childhood and early adolescence.