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Article Abstract

Tourette Syndrome (TS) and Persistent Tic Disorder (PTD) are childhood-onset neuropsychiatric conditions with high heritability. Due to current sample size limitations, identifying TS/PTD risk genes has been challenging. This study addressed this issue by conducting a meta-analysis of microarray copy number variant (CNV) studies from three TS/PTD genomics consortia, supplemented with new data from 3,291 cases. This approach more than doubled the sample size of previous TS/PTD CNV studies, with CNV calls generated from 5,725 TS/PTD cases and 10,982 matched controls. The results confirmed that TS/PTD cases 1) have a higher burden of ultra-rare deletions overlapping loss-of-function intolerant genes (OR = 1.68, P = 9.3×10^-5) and 2) are more likely to carry established neurodevelopmental CNVs (OR = 1.42, P = 3.9×10^-2) compared to controls. Additionally, a novel, genome-wide significant CNV locus for TS/PTD was discovered, involving duplications at 17q12 (hg19 chr17:34.8 - 36.2 Mb). This locus is associated with a known duplication syndrome associated with variable neuropsychiatric traits, but has not been previously linked to tic disorders. Eight cases and one control carried the canonical ~1.4 Mb duplication at chr17:34.8 - 36.2 Mb, while one additional case had a smaller 110 kb duplication within this known CNV that included only one gene, (acetyl-CoA carboxylase, OR = 26.7, P = 5.69×10^-7). Overall, this study provides further evidence that rare, genic CNVs play a substantial role in the genetic architecture of TS/PTD and identifies a new genome-wide significant association with this neurodevelopmental disorder.

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http://www.ncbi.nlm.nih.gov/pmc/articles/PMC12393602PMC
http://dx.doi.org/10.21203/rs.3.rs-7031850/v1DOI Listing

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