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Genetic analysis of activity, brain and behavioral associations in extended families with heavy genetic loading for bipolar disorder
Genetic analysis of activity, brain and behavioral associations in extended families with heavy genetic loading for bipolar disorder
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Genetic analysis of activity, brain and behavioral associations in extended families with heavy genetic loading for bipolar disorder
Genetic analysis of activity, brain and behavioral associations in extended families with heavy genetic loading for bipolar disorder

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Genetic analysis of activity, brain and behavioral associations in extended families with heavy genetic loading for bipolar disorder
Genetic analysis of activity, brain and behavioral associations in extended families with heavy genetic loading for bipolar disorder
Journal Article

Genetic analysis of activity, brain and behavioral associations in extended families with heavy genetic loading for bipolar disorder

2021
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Overview
Disturbed sleep and activity are prominent features of bipolar disorder type I (BP-I). However, the relationship of sleep and activity characteristics to brain structure and behavior in euthymic BP-I patients and their non-BP-I relatives is unknown. Additionally, underlying genetic relationships between these traits have not been investigated. Relationships between sleep and activity phenotypes, assessed using actigraphy, with structural neuroimaging (brain) and cognitive and temperament (behavior) phenotypes were investigated in 558 euthymic individuals from multi-generational pedigrees including at least one member with BP-I. Genetic correlations between actigraphy-brain and actigraphy-behavior associations were assessed, and bivariate linkage analysis was conducted for trait pairs with evidence of shared genetic influences. More physical activity and longer awake time were significantly associated with increased brain volumes and cortical thickness, better performance on neurocognitive measures of long-term memory and executive function, and less extreme scores on measures of temperament (impulsivity, cyclothymia). These associations did not differ between BP-I patients and their non-BP-I relatives. For nine activity-brain or activity-behavior pairs there was evidence for shared genetic influence (genetic correlations); of these pairs, a suggestive bivariate quantitative trait locus on chromosome 7 for wake duration and verbal working memory was identified. Our findings indicate that increased physical activity and more adequate sleep are associated with increased brain size, better cognitive function and more stable temperament in BP-I patients and their non-BP-I relatives. Additionally, we found evidence for pleiotropy of several actigraphy-behavior and actigraphy-brain phenotypes, suggesting a shared genetic basis for these traits.