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Haploinsufficiency in the ANKS1B gene encoding AIDA-1 leads to a neurodevelopmental syndrome

Author

Listed:
  • Abigail U. Carbonell

    (Albert Einstein College of Medicine)

  • Chang Hoon Cho

    (Albert Einstein College of Medicine)

  • Jaafar O. Tindi

    (Albert Einstein College of Medicine)

  • Pamela A. Counts

    (Albert Einstein College of Medicine)

  • Juliana C. Bates

    (Albert Einstein College of Medicine)

  • Hediye Erdjument-Bromage

    (New York University School of Medicine)

  • Svetlana Cvejic

    (Albert Einstein College of Medicine)

  • Alana Iaboni

    (Holland Bloorview Kids Rehabilitation Hospital)

  • Ifat Kvint

    (Hebrew University Hadassah Medical School)

  • Jenny Rosensaft

    (Hebrew University Hadassah Medical School)

  • Ehud Banne

    (Hebrew University Hadassah Medical School)

  • Evdokia Anagnostou

    (Holland Bloorview Kids Rehabilitation Hospital)

  • Thomas A. Neubert

    (New York University School of Medicine
    New York University School of Medicine)

  • Stephen W. Scherer

    (Hospital for Sick Children and University of Toronto)

  • Sophie Molholm

    (Albert Einstein College of Medicine
    Albert Einstein College of Medicine
    Albert Einstein College of Medicine)

  • Bryen A. Jordan

    (Albert Einstein College of Medicine
    Albert Einstein College of Medicine)

Abstract

Neurodevelopmental disorders, including autism spectrum disorder, have complex polygenic etiologies. Single-gene mutations in patients can help define genetic factors and molecular mechanisms underlying neurodevelopmental disorders. Here we describe individuals with monogenic heterozygous microdeletions in ANKS1B, a predicted risk gene for autism and neuropsychiatric diseases. Affected individuals present with a spectrum of neurodevelopmental phenotypes, including autism, attention-deficit hyperactivity disorder, and speech and motor deficits. Neurons generated from patient-derived induced pluripotent stem cells demonstrate loss of the ANKS1B-encoded protein AIDA-1, a brain-specific protein highly enriched at neuronal synapses. A transgenic mouse model of Anks1b haploinsufficiency recapitulates a range of patient phenotypes, including social deficits, hyperactivity, and sensorimotor dysfunction. Identification of the AIDA-1 interactome using quantitative proteomics reveals protein networks involved in synaptic function and the etiology of neurodevelopmental disorders. Our findings formalize a link between the synaptic protein AIDA-1 and a rare, previously undefined genetic disease we term ANKS1B haploinsufficiency syndrome.

Suggested Citation

  • Abigail U. Carbonell & Chang Hoon Cho & Jaafar O. Tindi & Pamela A. Counts & Juliana C. Bates & Hediye Erdjument-Bromage & Svetlana Cvejic & Alana Iaboni & Ifat Kvint & Jenny Rosensaft & Ehud Banne & , 2019. "Haploinsufficiency in the ANKS1B gene encoding AIDA-1 leads to a neurodevelopmental syndrome," Nature Communications, Nature, vol. 10(1), pages 1-15, December.
    • Handle: RePEc:nat:natcom:v:10:y:2019:i:1:d:10.1038_s41467-019-11437-w
    DOI: 10.1038/s41467-019-11437-w
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    Cited by:

    1. Chang Hoon Cho & Ilana Vasilisa Deyneko & Dylann Cordova-Martinez & Juan Vazquez & Anne S. Maguire & Jenny R. Diaz & Abigail U. Carbonell & Jaafar O. Tindi & Min-Hui Cui & Roman Fleysher & Sophie Molh, 2023. "ANKS1B encoded AIDA-1 regulates social behaviors by controlling oligodendrocyte function," Nature Communications, Nature, vol. 14(1), pages 1-20, December.

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