4.5 Article

2p15-p16.1 microdeletion syndrome: molecular characterization and association of the OTX1 and XPO1 genes with autism spectrum disorders

EUROPEAN JOURNAL OF HUMAN GENETICS (2011)

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EUROPEAN JOURNAL OF HUMAN GENETICS
卷 19, 期 12, 页码 1264-1270

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NATURE PUBLISHING GROUP
DOI: 10.1038/ejhg.2011.112

关键词

autism; real-time quantitative PCR; array comparative genomic hybridization; exportin 1 gene; orthodenticle homolog 1 gene

类别

Biochemistry & Molecular Biology Genetics & Heredity

资金

  1. Ontario Mental Health Foundation (OMHF)
  2. CIHR-IHRT [43820]
  3. ASD-CARC
  4. CIHR [RT-64217, MOP 74502]
  5. Michael Smith Foundation for Health Research
  6. New York State Office of Mental Retardation and Developmental Disabilities
  7. SIRFA network
  8. MIUR [2006058195]
  9. Italian Ministry of Health [RFPS-2007-5-640174]
  10. Autism Speaks Foundation

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Reports of unrelated individuals with autism spectrum disorder (ASD) and similar clinical features having overlapping de novo interstitial deletions at 2p15-p16.1 suggest that this region harbors a gene(s) important to the development of autism. We molecularly characterized two such deletions, selecting two genes in this region, exportin 1 (XPO1) and orthodenticle homolog 1 (OTX1) for association studies in three North American cohorts (Autism Spectrum Disorder -Canadian American Research Consortium (ASD-CARC), New York, and Autism Genetic Resource Exchange (AGRE)) and one Italian cohort (Societa Italiana per la Ricerca e la Formazione sull'Autismo (SIRFA)) of families with ASD. In XPO1, rs6735330 was associated with autism in all four cohorts (P<0.05), being significant in ASD-CARC cohorts (P-value following false discovery rate correction for multiple testing (P(FDR))=1.29 x 10(-5)), the AGRE cohort (P(FDR)=0.0011) and the combined families (P(FDR)=2.34 x 10(-9)). Similarly, in OTX1, rs2018650 and rs13000344 were associated with autism in ASD-CARC cohorts (P(FDR)=8.65 x 10(-7) and 6.07 x 10(5), respectively), AGRE cohort (P(FDR)=0.0034 and 0.015, respectively) and the combined families (P(FDR)=2.34 x 10(-9) and 0.00017, respectively); associations were marginal or insignificant in the New York and SIRFA cohorts. A significant association (P(FDR)=2.63 x 10(-11)) was found for the rs2018650G-rs13000344C haplotype. The above three SNPs were associated with severity of social interaction and verbal communication deficits and repetitive behaviors (P-values <0.01). No additional deletions were identified following screening of 798 ASD individuals. Our results indicate that deletion 2p15-p16.1 is not commonly associated with idiopathic ASD, but represents a novel contiguous gene syndrome associated with a constellation of phenotypic features (autism, intellectual disability, craniofacial/CNS dysmorphology), and that XPO1 and OXT1 may contribute to ASD in 2p15-p16.1 deletion cases and non-deletion cases of ASD mapping to this chromosome region. European Journal of Human Genetics (2011) 19, 1264-1270; doi: 10.1038/ejhg.2011.112; published online 13 July 2011

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