Biallelic mutations in the death domain of PIDD1 impair caspase-2 activation and are associated with intellectual disability.

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Abstrakt

Tytuł:: Biallelic mutations in the death domain of PIDD1 impair caspase-2 activation and are associated with intellectual disability.
Autorzy:: Sheikh TI; Molecular Neuropsychiatry & Development (MiND) Lab, Campbell Family Mental Health Research Institute, Centre for Addiction and Mental Health, Toronto, ON, M5T 1R8, Canada.; Institute of Medical Science, University of Toronto, Toronto, ON, Canada.; Molecular Genetics Laboratory, North York General Hosptial Genetics Program, Toronto, ON, M2K 1E1, Canada.
Vasli N; Molecular Neuropsychiatry & Development (MiND) Lab, Campbell Family Mental Health Research Institute, Centre for Addiction and Mental Health, Toronto, ON, M5T 1R8, Canada.
Pastore S; Molecular Neuropsychiatry & Development (MiND) Lab, Campbell Family Mental Health Research Institute, Centre for Addiction and Mental Health, Toronto, ON, M5T 1R8, Canada.; Institute of Medical Science, University of Toronto, Toronto, ON, Canada.
Kharizi K; Genetics Research Center, University of Social Welfare and Rehabilitation Sciences, Tehran, 19834, Iran.
Harripaul R; Molecular Neuropsychiatry & Development (MiND) Lab, Campbell Family Mental Health Research Institute, Centre for Addiction and Mental Health, Toronto, ON, M5T 1R8, Canada.; Institute of Medical Science, University of Toronto, Toronto, ON, Canada.
Fattahi Z; Genetics Research Center, University of Social Welfare and Rehabilitation Sciences, Tehran, 19834, Iran.
Pande S; Department of Medical Genetics, Kasturba Medical College, Manipal, Manipal Academy of Higher Education, Manipal, Karnataka, 576104, India.
Naeem F; General and Health Systems Psychiatry, Centre for Addiction and Mental Health, Toronto, ON, M5T 1R8, Canada.; Department of Psychiatry, University of Toronto, Toronto, ON, M5T 1R8, Canada.
Hussain A; Human Molecular Genetics Lab, Department of Biological Sciences, FBAS, International Islamic University, Islamabad, Pakistan.
Mir A; Human Molecular Genetics Lab, Department of Biological Sciences, FBAS, International Islamic University, Islamabad, Pakistan.
Islam O; Department of Diagnostic Radiology, Queens University, Kingston, ON, K7L 2V7, Canada.
Girisha KM; Department of Medical Genetics, Kasturba Medical College, Manipal, Manipal Academy of Higher Education, Manipal, Karnataka, 576104, India.
Irfan M; Department of Mental Health, Psychiatry and Behavioural Sciences, Peshawar Medical College, Riphah International University, Islamabad, Pakistan.
Ayub M; Lahore Institute of Research & Development, Lahore, 51000, Pakistan.; Department of Psychiatry, Queen's University, Kingston, ON, K7L 3N6, Canada.
Schwarzer C; Department of Pharmacology, Medical University of Innsbruck, Innsbruck, Austria.
Najmabadi H; Genetics Research Center, University of Social Welfare and Rehabilitation Sciences, Tehran, 19834, Iran.; Kariminejad-Najmabadi Pathology and Genetics Center, Tehran, 14667, Iran.
Shukla A; Department of Medical Genetics, Kasturba Medical College, Manipal, Manipal Academy of Higher Education, Manipal, Karnataka, 576104, India.
Sladky VC; Institute for Developmental Immunology, Biocenter Medical University of Innsbruck, Innsbruck, Austria.
Braun VZ; Institute for Developmental Immunology, Biocenter Medical University of Innsbruck, Innsbruck, Austria.
Garcia-Carpio I; Institute for Developmental Immunology, Biocenter Medical University of Innsbruck, Innsbruck, Austria.
Villunger A; Institute for Developmental Immunology, Biocenter Medical University of Innsbruck, Innsbruck, Austria. .; CeMM Research Center for Molecular Medicine of the Austrian Academy of Sciences, Vienna, Austria. .; Ludwig Boltzmann Institute for Rare and Undiagnosed Diseases, Vienna, Austria. .
Vincent JB; Molecular Neuropsychiatry & Development (MiND) Lab, Campbell Family Mental Health Research Institute, Centre for Addiction and Mental Health, Toronto, ON, M5T 1R8, Canada. .; Institute of Medical Science, University of Toronto, Toronto, ON, Canada. .; Department of Psychiatry, University of Toronto, Toronto, ON, M5T 1R8, Canada. .
Źródło:: Translational psychiatry [Transl Psychiatry] 2021 Jan 05; Vol. 11 (1), pp. 1. Date of Electronic Publication: 2021 Jan 05.
Typ publikacji:: Journal Article; Research Support, N.I.H., Extramural; Research Support, Non-U.S. Gov't
Język:: English
Imprint Name(s):: Original Publication: New York, NY : Nature Pub. Group
MeSH Terms:: CRADD Signaling Adaptor Protein*/genetics
CRADD Signaling Adaptor Protein*/metabolism
Intellectual Disability*/genetics
Animals ; Caspase 2/genetics ; Caspase 2/metabolism ; Death Domain ; Death Domain Receptor Signaling Adaptor Proteins/genetics ; HEK293 Cells ; Humans ; India ; Mice ; Mutation
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Grant Information:: 1R01HD093570-01A1 International U.S. Department of Health & Human Services | NIH | Center for Information Technology (Center for Information Technology, National Institutes of Health); POLICE International EC | EU Framework Programme for Research and Innovation H2020 | H2020 Priority Excellent Science | H2020 European Research Council (H2020 Excellent Science - European Research Council); MOP-102758 International Gouvernement du Canada | Canadian Institutes of Health Research (Instituts de Recherche en Santé du Canada); 920384578 International Iran National Science Foundation (INSF); n/a International Brain and Behavior Research Foundation (Brain & Behavior Research Foundation); FWF (PIR-3) International Austrian Science Fund (Fonds zur Förderung der Wissenschaftlichen Forschung); R01 HD093570 United States HD NICHD NIH HHS; PJT-156402 International Gouvernement du Canada | Canadian Institutes of Health Research (Instituts de Recherche en Santé du Canada)
Substance Nomenclature:: 0 (CRADD Signaling Adaptor Protein)
0 (Death Domain Receptor Signaling Adaptor Proteins)
0 (PIDD1 protein, human)
0 (Pidd1 protein, mouse)
EC 3.4.22.- (Caspase 2)
Entry Date(s):: Date Created: 20210108 Date Completed: 20210618 Latest Revision: 20240330
Update Code:: 20240330
PubMed Central ID:: PMC7791037
DOI:: 10.1038/s41398-020-01158-w
PMID:: 33414379
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PIDD1 encodes p53-Induced Death Domain protein 1, which acts as a sensor surveilling centrosome numbers and p53 activity in mammalian cells. Early results also suggest a role in DNA damage response where PIDD1 may act as a cell-fate switch, through interaction with RIP1 and NEMO/IKKg, activating NF-κB signaling for survival, or as an apoptosis-inducing protein by activating caspase-2. Biallelic truncating mutations in CRADD-the protein bridging PIDD1 and caspase-2-have been reported in intellectual disability (ID), and in a form of lissencephaly. Here, we identified five families with ID from Iran, Pakistan, and India, with four different biallelic mutations in PIDD1, all disrupting the Death Domain (DD), through which PIDD1 interacts with CRADD or RIP1. Nonsense mutations Gln863* and Arg637* directly disrupt the DD, as does a missense mutation, Arg815Trp. A homozygous splice mutation in the fifth family is predicted to disrupt splicing upstream of the DD, as confirmed using an exon trap. In HEK293 cells, we show that both Gln863* and Arg815Trp mutants fail to co-localize with CRADD, leading to its aggregation and mis-localization, and fail to co-precipitate CRADD. Using genome-edited cell lines, we show that these three PIDD1 mutations all cause loss of PIDDosome function. Pidd1 null mice show decreased anxiety, but no motor abnormalities. Together this indicates that PIDD1 mutations in humans may cause ID (and possibly lissencephaly) either through gain of function or secondarily, due to altered scaffolding properties, while complete loss of PIDD1, as modeled in mice, may be well tolerated or is compensated for.

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