Abstract
Neurodevelopmental problems (NPs) are more common in males, whereas anxiety and depression are more common in females. Rare copy number variants (CNVs) have been implicated in neurodevelopmental disorders. The aim of this study was to characterize the relationship between rare CNVs with NPs, anxiety, and depression in a childhood population sample, as well as to examine sex‐specific effects. We analyzed a sample of N = 12,982 children, of whom 5.3% had narrowly defined NPs (clinically diagnosed), 20.9% had broadly defined NPs (based on validated screening measures, but no diagnosis), and 3.0% had clinically diagnosed anxiety or depression. Rare (<1% frequency) CNVs were categorized by size (100–500 kb or > 500 kb), type, and putative relevance to NPs. We tested for association of CNV categories with outcomes and examined sex‐specific effects. Medium deletions (OR[CI] = 1.18[1.05–1.33], p = .0053) and large duplications (OR[CI] = 1.45[1.19–1.75], p = .00017) were associated with broadly defined NPs. Large deletions (OR[CI] = 1.85[1.14–3.01], p = .013) were associated with narrowly defined NPs. There were no significant sex differences in CNV burden in individuals with NPs. Although CNVs were not associated with anxiety/depression in the whole sample, in individuals diagnosed with these disorders, females were more likely to have large CNVs (OR[CI] = 3.75[1.45–9.68], p = .0064). Rare CNVs are associated with both narrowly and broadly defined NPs in a general population sample of children. Our results also suggest that large, rare CNVs may show sex‐specific phenotypic effects.
Highlights
We examined the overall association of all copy number variants (CNVs) passing quality control (QC), with narrowly and broadly defined Neurodevelopmental problems (NPs), as well as with clinically defined anxiety/depression
We extend this knowledge by implicating rare CNVs in children with more broadly defined, subthreshold NPs and continuously assessed traits of broad NPs, which has not been shown before
We found no association between rare CNVs and clinically diagnosed anxiety and depression in this childhood sample, in line with a recent childhood population study (Guyatt et al, 2018), albeit in contrast to a population study which found an association between neuropsychiatric CNVs and depression in adults (Stefansson et al, 2014)
Summary
The effect sizes for the association of CNV classes with ASD and large duplications with tics were similar to the analyses of ADHD and learning difficulties, these results did not reach significance (see Supporting Information Table S4).
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More From: American Journal of Medical Genetics Part B: Neuropsychiatric Genetics
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