Convergence of Genes and Cellular Pathways Dysregulated in Autism Spectrum Disorders

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• 作者：Dalila Pintop>1p>p> ; p>p>2p>p> ; p>p>3p>p> ; p>p>4p>p> ; p>p>5p>p> ; p>p>6p>p> ; p>p>85p> ; Elsa Delabyp>7p>p> ; p>p>8p>p> ; p>p>9p> ; Daniele Mericop>10p> ; Mafalda Barbosap>1p>p> ; p>p>2p>p> ; p>p>3p>p> ; p>p>4p> ; Alison Merikangasp>11p> ; Lambertus Kleip>12p> ; Bhooma Thiruvahindrapuramp>10p> ; Xiao Xup>2p>p> ; p>p>4p>p> ; p>p>5p> ; Robert Zimanp>10p> ; Zhuozhi Wangp>10p> ; Jacob A.S. Vorstmanp>13p> ; Ann Thompsonp>14p> ; Regina Reganp>15p>p> ; p>p>16p> ; Marion Pilorgep>7p>p> ; p>p>8p>p> ; p>p>9p> ; Giovanna Pellecchiap>10p> ; Alistair T. Pagnamentap>17p> ; Bá ; rbara Oliveirap>18p>p> ; p>p>19p> ; Christian R. Marshallp>10p>p> ; p>p>20p> ; Tiago R. Magalhaesp>15p>p> ; p>p>16p> ; Jennifer K. Lowep>21p> ; Jennifer L. Howep>10p> ; Anthony J. Griswoldp>22p> ; John Gilbertp>22p> ; Eftichia Duketisp>23p> ; Beth A. Dombroskip>24p> ; Maretha V. De Jongep>13p> ; Michael Cuccarop>22p> ; Emily L. Crawfordp>25p> ; Catarina T. Correiap>18p>p> ; p>p>19p> ; Judith Conroyp>16p>p> ; p>p>26p> ; Inê ; s C. Conceiç ; ã ; op>18p>p> ; p>p>19p> ; Andreas G. Chiocchettip>23p> ; Jillian P. Caseyp>15p>p> ; p>p>16p> ; Guiqing Caip>1p>p> ; p>p>2p>p> ; p>p>3p> ; Christelle Cabrolp>7p>p> ; p>p>8p>p> ; p>p>9p> ; Nadia Bolshakovap>11p> ; Elena Bacchellip>27p> ; Richard Anneyp>11p> ; Steven Gallingerp>28p> ; Michelle Cotterchiop>29p> ; Graham Caseyp>30p> ; Lonnie Zwaigenbaump>31p> ; Kerstin Wittemeyerp>32p> ; Kirsty Wingp>17p> ; Simon Wallacep>33p> ; Herman van Engelandp>13p> ; Ana Tryfonp>1p>p> ; p>p>2p>p> ; p>p>80p> ; Susanne Thomsonp>25p> ; Latha Sooryap>1p>p> ; p>p>2p>p> ; p>p>81p> ; Bernadette Rogé ; p>34p> ; Wendy Robertsp>35p> ; Fritz Poustkap>23p> ; Susana Mougap>36p>p> ; p>p>37p> ; Nancy Minshewp>12p> ; L. Alison McInnesp>1p>p> ; p>p>2p>p> ; p>p>82p> ; Susan G. McGrewp>38p> ; Catherine Lordp>39p> ; Marion Leboyerp>40p>p> ; p>p>41p>p> ; p>p>42p>p> ; p>p>43p> ; Ann S. Le Couteurp>44p> ; Alexander Kolevzonp>1p>p> ; p>p>2p>p> ; p>p>6p> ; Patricia Jimé ; nez Gonzá ; lezp>45p> ; Suma Jacobp>46p>p> ; p>p>47p> ; Richard Holtp>17p> ; Stephen Guterp>46p> ; Jonathan Greenp>48p>p> ; p>p>49p> ; Andrew Greenp>16p>p> ; p>p>50p> ; Christopher Gillbergp>51p> ; Bridget A. Fernandezp>52p> ; Frederico Duquep>36p>p> ; p>p>37p> ; Richard Delormep>40p>p> ; p>p>53p>p> ; p>p>54p>p> ; p>p>55p> ; Geraldine Dawsonp>56p> ; Pauline Chastep>12p>p> ; p>p>40p> ; Cá ; tia Café ; p>36p> ; Sean Brennanp>11p> ; Thomas Bourgeronp>40p>p> ; p>p>53p>p> ; p>p>54p>p> ; p>p>57p> ; Patrick F. Boltonp>58p>p> ; p>p>59p> ; Sven Bö ; ltep>60p>p> ; p>p>83p> ; Raphael Bernierp>61p> ; Gillian Bairdp>62p> ; Anthony J. Baileyp>33p>p> ; p>p>84p> ; Evdokia Anagnostoup>63p> ; Joana Almeidap>36p> ; Ellen M. Wijsmanp>64p>p> ; p>p>65p> ; Veronica J. Vielandp>66p> ; Astrid M. Vicentep>18p>p> ; p>p>19p> ; Gerard D. Schellenbergp>24p> ; Margaret Pericak-Vancep>22p> ; Andrew D. Patersonp>10p>p> ; p>p>67p> ; Jeremy R. Parrp>68p> ; Guiomar Oliveirap>36p>p> ; p>p>37p> ; John I. Nurnbergerp>69p>p> ; p>p>70p> ; Anthony P. Monacop>17p>p> ; p>p>71p> ; Elena Maestrinip>27p> ; Sabine M. Klauckp>72p> ; Hakon Hakonarsonp>73p>p> ; p>p>74p> ; Jonathan L. Hainesp>25p> ; Daniel H. Geschwindp>21p> ; Christine M. Freitagp>23p> ; Susan E. Folsteinp>75p> ; Sean Ennisp>16p>p> ; p>p>50p> ; Hilary Coonp>76p> ; Agatino Battagliap>77p> ; Peter Szatmarip>14p> ; James S. Sutcliffep>25p> ; Joachim Hallmayerp>78p> ; Michael Gillp>11p> ; Edwin H. Cookp>46p> ; Joseph D. Buxbaump>1p>p> ; p>p>2p>p> ; p>p>3p>p> ; p>p>4p>p> ; p>p>6p>p> ; p>p>79p> ; Bernie Devlinp>12p> ; Louise Gallagherp>11p> ; Catalina Betancurp>7p>p> ; p>p>8p>p> ; p>p>9p>p> ; p>p>85p>p> ; p>p>catalina.betancur@inserm.fr" class="auth_mailp> ; Stephen W. Schererp>10p>p> ; p>p>20p>p> ; p>p>85p>p> ; p>p>stephen.scherer@sickkids.ca" class="auth_mailp>
• 刊名：The American Journal of Human Genetics
• 出版年：1 May 2014
• 年：2014
• 卷：94
• 期：5
• 页码：677-694
• 全文大小：1043 K

文摘

Rare copy-number variation (CNV) is an important source of risk for autism spectrum disorders (ASDs). We analyzed 2,446 ASD-affected families and confirmed an excess of genic deletions and duplications in affected versus control groups (1.41-fold, p = 1.0 × 10p>−5p>) and an increase in affected subjects carrying exonic pathogenic CNVs overlapping known loci associated with dominant or X-linked ASD and intellectual disability (odds ratio = 12.62, p = 2.7 × 10p>−15p>, ∼3% of ASD subjects). Pathogenic CNVs, often showing variable expressivity, included rare de novo and inherited events at 36 loci, implicating ASD-associated genes (CHD2, HDAC4, and GDI1) previously linked to other neurodevelopmental disorders, as well as other genes such as SETD5, MIR137, and HDAC9. Consistent with hypothesized gender-specific modulators, females with ASD were more likely to have highly penetrant CNVs (p = 0.017) and were also overrepresented among subjects with fragile X syndrome protein targets (p = 0.02). Genes affected by de novo CNVs and/or loss-of-function single-nucleotide variants converged on networks related to neuronal signaling and development, synapse function, and chromatin regulation.