论文信息 - Exome sequencing of extended families with autism reveals genes shared across neurodevelopmental and neuropsychiatric disorders

Exome sequencing of extended families with autism reveals genes shared across neurodevelopmental and neuropsychiatric disorders

BackgroundAutism spectrum disorders (ASDs) comprise a range of neurodevelopmental conditions of varying severity, characterized by marked qualitative difficulties in social relatedness, communication, and behavior. Despite overwhelming evidence of high heritability, results from genetic studies to date show that ASD etiology is extremely heterogeneous and only a fraction of autism genes have been discovered.MethodsTo help unravel this genetic complexity, we performed whole exome sequencing on 100 ASD individuals from 40 families with multiple distantly related affected individuals. All families contained a minimum of one pair of ASD cousins. Each individual was captured with the Agilent SureSelect Human All Exon kit, sequenced on the Illumina Hiseq 2000, and the resulting data processed and annotated with Burrows-Wheeler Aligner (BWA), Genome Analysis Toolkit (GATK), and SeattleSeq. Genotyping information on each family was utilized in order to determine genomic regions that were identical by descent (IBD). Variants identified by exome sequencing which occurred in IBD regions and present in all affected individuals within each family were then evaluated to determine which may potentially be disease related. Nucleotide alterations that were novel and rare (minor allele frequency, MAF, less than 0.05) and predicted to be detrimental, either by altering amino acids or splicing patterns, were prioritized.ResultsWe identified numerous potentially damaging, ASD associated risk variants in genes previously unrelated to autism. A subset of these genes has been implicated in other neurobehavioral disorders including depression (SLIT3), epilepsy (CLCN2, PRICKLE1), intellectual disability (AP4M1), schizophrenia (WDR60), and Tourette syndrome (OFCC1). Additional alterations were found in previously reported autism candidate genes, including three genes with alterations in multiple families (CEP290, CSMD1, FAT1, and STXBP5). Compiling a list of ASD candidate genes from the literature, we determined that variants occurred in ASD candidate genes 1.65 times more frequently than in random genes captured by exome sequencing (P = 8.55 × 10-5).ConclusionsBy studying these unique pedigrees, we have identified novel DNA variations related to ASD, demonstrated that exome sequencing in extended families is a powerful tool for ASD candidate gene discovery, and provided further evidence of an underlying genetic component to a wide range of neurodevelopmental and neuropsychiatric diseases.

[1] Robert T. Schultz,et al. Autism genome-wide copy number variation reveals ubiquitin and neuronal genes , 2009, Nature.

[2] Jun Aruga,et al. Dorz1, a novel gene expressed in differentiating cerebellar granule neurons, is down-regulated in Zic1-deficient mouse. , 2003, Brain research. Molecular brain research.

[3] V. Sheffield,et al. Novel copy number variants in children with autism and additional developmental anomalies , 2009, Journal of Neurodevelopmental Disorders.

[4] M. Behen,et al. Exome sequencing of a pedigree with tourette syndrome or chronic tic disorder , 2011, Annals of neurology.

[5] M J Owen,et al. Positional cloning, association analysis and expression studies provide convergent evidence that the cadherin gene FAT contains a bipolar disorder susceptibility allele , 2006, Molecular Psychiatry.

[6] Joanne M. Britto,et al. Sez-6 Proteins Affect Dendritic Arborization Patterns and Excitability of Cortical Pyramidal Neurons , 2007, Neuron.

[7] M. DePristo,et al. The Genome Analysis Toolkit: a MapReduce framework for analyzing next-generation DNA sequencing data. , 2010, Genome research.

[8] L. Tsai,et al. Validation of schizophrenia-associated genes CSMD1, C10orf26, CACNA1C and TCF4 as miR-137 targets , 2013, Molecular Psychiatry.

[9] Scott M. Williams,et al. Copy Number Variants in Extended Autism Spectrum Disorder Families Reveal Candidates Potentially Involved in Autism Risk , 2011, PloS one.

[10] Gary D Bader,et al. Functional impact of global rare copy number variation in autism spectrum disorders , 2010, Nature.

[11] S. Bölte,et al. Autism Diagnostic Interview-Revised (ADI-R) Algorithms for Toddlers and Young Preschoolers: Application in a Non-US Sample of 1,104 Children , 2015, Journal of Autism and Developmental Disorders.

[12] Laurence Faivre,et al. Recurrent rearrangements in synaptic and neurodevelopmental genes and shared biologic pathways in schizophrenia, autism, and mental retardation. , 2009, Archives of general psychiatry.

[13] M. Yuzaki. The Ins and Outs of GluD2—Why and How Purkinje Cells Use the Special Glutamate Receptor , 2011, The Cerebellum.

[14] Joseph T. Glessner,et al. A novel approach of homozygous haplotype sharing identifies candidate genes in autism spectrum disorder , 2011, Human Genetics.

[15] Kristian Cibulskis,et al. A homozygous missense mutation in HERC2 associated with global developmental delay and autism spectrum disorder , 2012, Human mutation.

[16] Pat Levitt,et al. The conundrums of understanding genetic risks for autism spectrum disorders , 2011, Nature Neuroscience.

[17] Robert T. Schultz,et al. Common genetic variants on 5p14.1 associate with autism spectrum disorders , 2009, Nature.

[18] M. Nöthen,et al. Adaptor protein complex 4 deficiency causes severe autosomal-recessive intellectual disability, progressive spastic paraplegia, shy character, and short stature. , 2011, American journal of human genetics.

[19] F. Coppieters,et al. CEP290, a gene with many faces: mutation overview and presentation of CEP290base , 2010, Human mutation.

[20] J. Gilbert,et al. A Genome‐wide Association Study of Autism Reveals a Common Novel Risk Locus at 5p14.1 , 2009, Annals of human genetics.

[21] John J. Connolly,et al. The Genetics of Autism Spectrum Disorders , 2011 .

[22] J. Goodship,et al. Identification of a mutation in synapsin I, a synaptic vesicle protein, in a family with epilepsy , 2004, Journal of Medical Genetics.

[23] Timothy W. Yu,et al. Whole-Exome Sequencing and Homozygosity Analysis Implicate Depolarization-Regulated Neuronal Genes in Autism , 2012, PLoS genetics.

[24] P. Shannon,et al. Exome sequencing identifies the cause of a Mendelian disorder , 2009, Nature Genetics.

[25] M. Owen,et al. Genetic overlap between autism, schizophrenia and bipolar disorder , 2009, Genome Medicine.

[26] D. Pinto,et al. Structural variation of chromosomes in autism spectrum disorder. , 2008, American journal of human genetics.

[27] B. Ritz,et al. Gain-of-function variant in GLUD2 glutamate dehydrogenase modifies Parkinson's disease onset , 2010, European Journal of Human Genetics.

[28] Lin-Tao Zhou,et al. Febrile seizures are associated with mutation of seizure‐related (SEZ) 6, a brain‐specific gene , 2007, Journal of neuroscience research.

[29] Kenny Q. Ye,et al. De Novo Gene Disruptions in Children on the Autistic Spectrum , 2012, Neuron.

[30] Joseph T. Glessner,et al. Rare Copy Number Variants in Tourette Syndrome Disrupt Genes in Histaminergic Pathways and Overlap with Autism , 2012, Biological Psychiatry.

[31] Shuwen Huang,et al. Transmitted duplication of 8p23.1–8p23.2 associated with speech delay, autism and learning difficulties , 2009, European Journal of Human Genetics.

[32] C. Shaw,et al. Exercise and Genetic Rescue of SCA1 via the Transcriptional Repressor Capicua , 2011, Science.

[33] J. Piven,et al. Evaluation of the chromosome 2q37.3 gene CENTG2 as an autism susceptibility gene , 2005, American journal of medical genetics. Part B, Neuropsychiatric genetics : the official publication of the International Society of Psychiatric Genetics.

[34] G. Abecasis,et al. Merlin—rapid analysis of dense genetic maps using sparse gene flow trees , 2002, Nature Genetics.

[35] M. Scott,et al. A homozygous mutation in human PRICKLE1 causes an autosomal-recessive progressive myoclonus epilepsy-ataxia syndrome. , 2008, American journal of human genetics.

[36] Vinit B. Mahajan,et al. PRICKLE1 Interaction with SYNAPSIN I Reveals a Role in Autism Spectrum Disorders , 2013, PloS one.

[37] Manuel A. R. Ferreira,et al. PLINK: a tool set for whole-genome association and population-based linkage analyses. , 2007, American journal of human genetics.

[38] Bradley P. Coe,et al. Sporadic autism exomes reveal a highly interconnected protein network of de novo mutations , 2012, Nature.

[39] M. DePristo,et al. A framework for variation discovery and genotyping using next-generation DNA sequencing data , 2011, Nature Genetics.

[40] P Ferrara,et al. Neurotensin is an antagonist of the human neurotensin NT2 receptor expressed in Chinese hamster ovary cells. , 1998, European journal of pharmacology.

[41] R. Hu. Diagnostic and Statistical Manual of Mental Disorders (DSM-IV) , 2003 .

[42] P. Bork,et al. A method and server for predicting damaging missense mutations , 2010, Nature Methods.

[43] John Wei,et al. Identify Risk Genes for ADHD Rare Copy Number Variation Discovery and Cross-Disorder Comparisons , 2011 .

[44] Daniel H. Geschwind,et al. Genetics of autism spectrum disorders , 2011, Trends in Cognitive Sciences.

[45] Vidar M. Steen,et al. The Complement Control-Related Genes CSMD1 and CSMD2 Associate to Schizophrenia , 2011, Biological Psychiatry.