PRICKLE2 revisited—further evidence implicating PRICKLE2 in neurodevelopmental disorders

PRICKLE2 encodes a member of a highly conserved family of proteins that are involved in the non-canonical Wnt and planar cell polarity signaling pathway. Prickle2 localizes to the post-synaptic density, and interacts with post-synaptic density protein 95 and the NMDA receptor. Loss-of-function varia...

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Published in	European journal of human genetics : EJHG Vol. 29; no. 8; pp. 1235 - 1244
Main Authors	Bayat, Allan, Iqbal, Sumaiya, Borredy, Kim, Amiel, Jeanne, Zweier, Christiane, Barcia, Guilia, Kraus, Cornelia, Weyhreter, Heike, Bassuk, Alexander G., Chopra, Maya, Rubboli, Guido, Møller, Rikke S.
Format	Journal Article
Language	English
Published	England Nature Publishing Group 01.08.2021 Springer International Publishing
Subjects	Adolescent Adult Aged Amino acids Autism Child Codon, Nonsense Computational neuroscience Convulsions & seizures Developmental Disabilities - genetics Developmental Disabilities - pathology Epilepsy Female Frameshift Mutation Genetics Glutamic acid receptors (ionotropic) Hospitals Human subjects Humans LIM Domain Proteins - chemistry LIM Domain Proteins - genetics Male Membrane Proteins - chemistry Membrane Proteins - genetics Mutation, Missense N-Methyl-D-aspartic acid receptors Neurodevelopmental disorders Pathogenicity Pediatrics Phenotype Phenotypes Polarity Protein Domains Proteins Seizures Signal transduction Synaptic density Wnt protein
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Abstract	PRICKLE2 encodes a member of a highly conserved family of proteins that are involved in the non-canonical Wnt and planar cell polarity signaling pathway. Prickle2 localizes to the post-synaptic density, and interacts with post-synaptic density protein 95 and the NMDA receptor. Loss-of-function variants in prickle2 orthologs cause seizures in flies and mice but evidence for the role of PRICKLE2 in human disease is conflicting. Our goal is to provide further evidence for the role of this gene in humans and define the phenotypic spectrum of PRICKLE2-related disorders. We report a cohort of six subjects from four unrelated families with heterozygous rare PRICKLE2 variants (NM_198859.4). Subjects were identified through an international collaboration. Detailed phenotypic and genetic assessment of the subjects were carried out and in addition, we assessed the variant pathogenicity using bioinformatic approaches. We identified two missense variants (c.122 C > T; p.(Pro41Leu), c.680 C > G; p.(Thr227Arg)), one nonsense variant (c.214 C > T; p.(Arg72) and one frameshift variant (c.1286_1287delGT; p.(Ser429Thrfs56)). While the p.(Ser429Thrfs*56) variant segregated with disease in a family with three affected females, the three remaining variants occurred de novo. Subjects shared a mild phenotype characterized by global developmental delay, behavioral difficulties ± epilepsy, autistic features, and attention deficit hyperactive disorder. Computational analysis of the missense variants suggest that the altered amino acid residues are likely to be located in protein regions important for function. This paper demonstrates that PRICKLE2 is involved in human neuronal development and that pathogenic variants in PRICKLE2 cause neurodevelopmental delay, behavioral difficulties and epilepsy in humans.
AbstractList	PRICKLE2 encodes a member of a highly conserved family of proteins that are involved in the non-canonical Wnt and planar cell polarity signaling pathway. Prickle2 localizes to the post-synaptic density, and interacts with post-synaptic density protein 95 and the NMDA receptor. Loss-of-function variants in prickle2 orthologs cause seizures in flies and mice but evidence for the role of PRICKLE2 in human disease is conflicting. Our goal is to provide further evidence for the role of this gene in humans and define the phenotypic spectrum of PRICKLE2-related disorders. We report a cohort of six subjects from four unrelated families with heterozygous rare PRICKLE2 variants (NM_198859.4). Subjects were identified through an international collaboration. Detailed phenotypic and genetic assessment of the subjects were carried out and in addition, we assessed the variant pathogenicity using bioinformatic approaches. We identified two missense variants (c.122 C > T; p.(Pro41Leu), c.680 C > G; p.(Thr227Arg)), one nonsense variant (c.214 C > T; p.(Arg72) and one frameshift variant (c.1286_1287delGT; p.(Ser429Thrfs56)). While the p.(Ser429Thrfs56) variant segregated with disease in a family with three affected females, the three remaining variants occurred de novo. Subjects shared a mild phenotype characterized by global developmental delay, behavioral difficulties ± epilepsy, autistic features, and attention deficit hyperactive disorder. Computational analysis of the missense variants suggest that the altered amino acid residues are likely to be located in protein regions important for function. This paper demonstrates that PRICKLE2 is involved in human neuronal development and that pathogenic variants in PRICKLE2 cause neurodevelopmental delay, behavioral difficulties and epilepsy in humans. PRICKLE2 encodes a member of a highly conserved family of proteins that are involved in the non-canonical Wnt and planar cell polarity signaling pathway. Prickle2 localizes to the post-synaptic density, and interacts with post-synaptic density protein 95 and the NMDA receptor. Loss-of-function variants in prickle2 orthologs cause seizures in flies and mice but evidence for the role of PRICKLE2 in human disease is conflicting. Our goal is to provide further evidence for the role of this gene in humans and define the phenotypic spectrum of PRICKLE2- related disorders. We report a cohort of six subjects from four unrelated families with heterozygous rare PRICKLE2 variants (NM_198859.4). Subjects were identified through an international collaboration. Detailed phenotypic and genetic assessment of the subjects were carried out and in addition, we assessed the variant pathogenicity using bioinformatic approaches. We identified two missense variants (c.122 C > T; p.(Pro41Leu), c.680 C > G; p.(Thr227Arg)), one nonsense variant (c.214 C > T; p.(Arg72) and one frameshift variant (c.1286_1287delGT; p.(Ser429Thrfs56)). While the p.(Ser429Thrfs56) variant segregated with disease in a family with three affected females, the three remaining variants occurred de novo. Subjects shared a mild phenotype characterized by global developmental delay, behavioral difficulties ± epilepsy, autistic features, and attention deficit hyperactive disorder. Computational analysis of the missense variants suggest that the altered amino acid residues are likely to be located in protein regions important for function. This paper demonstrates that PRICKLE2 is involved in human neuronal development and that pathogenic variants in PRICKLE2 cause neurodevelopmental delay, behavioral difficulties and epilepsy in humans. PRICKLE2 encodes a member of a highly conserved family of proteins that are involved in the non-canonical Wnt and planar cell polarity signaling pathway. Prickle2 localizes to the post-synaptic density, and interacts with post-synaptic density protein 95 and the NMDA receptor. Loss-of-function variants in prickle2 orthologs cause seizures in flies and mice but evidence for the role of PRICKLE2 in human disease is conflicting. Our goal is to provide further evidence for the role of this gene in humans and define the phenotypic spectrum of PRICKLE2-related disorders. We report a cohort of six subjects from four unrelated families with heterozygous rare PRICKLE2 variants (NM_198859.4). Subjects were identified through an international collaboration. Detailed phenotypic and genetic assessment of the subjects were carried out and in addition, we assessed the variant pathogenicity using bioinformatic approaches. We identified two missense variants (c.122 C > T; p.(Pro41Leu), c.680 C > G; p.(Thr227Arg)), one nonsense variant (c.214 C > T; p.(Arg72) and one frameshift variant (c.1286_1287delGT; p.(Ser429Thrfs56)). While the p.(Ser429Thrfs56) variant segregated with disease in a family with three affected females, the three remaining variants occurred de novo. Subjects shared a mild phenotype characterized by global developmental delay, behavioral difficulties ± epilepsy, autistic features, and attention deficit hyperactive disorder. Computational analysis of the missense variants suggest that the altered amino acid residues are likely to be located in protein regions important for function. This paper demonstrates that PRICKLE2 is involved in human neuronal development and that pathogenic variants in PRICKLE2 cause neurodevelopmental delay, behavioral difficulties and epilepsy in humans.PRICKLE2 encodes a member of a highly conserved family of proteins that are involved in the non-canonical Wnt and planar cell polarity signaling pathway. Prickle2 localizes to the post-synaptic density, and interacts with post-synaptic density protein 95 and the NMDA receptor. Loss-of-function variants in prickle2 orthologs cause seizures in flies and mice but evidence for the role of PRICKLE2 in human disease is conflicting. Our goal is to provide further evidence for the role of this gene in humans and define the phenotypic spectrum of PRICKLE2-related disorders. We report a cohort of six subjects from four unrelated families with heterozygous rare PRICKLE2 variants (NM_198859.4). Subjects were identified through an international collaboration. Detailed phenotypic and genetic assessment of the subjects were carried out and in addition, we assessed the variant pathogenicity using bioinformatic approaches. We identified two missense variants (c.122 C > T; p.(Pro41Leu), c.680 C > G; p.(Thr227Arg)), one nonsense variant (c.214 C > T; p.(Arg72) and one frameshift variant (c.1286_1287delGT; p.(Ser429Thrfs56)). While the p.(Ser429Thrfs56) variant segregated with disease in a family with three affected females, the three remaining variants occurred de novo. Subjects shared a mild phenotype characterized by global developmental delay, behavioral difficulties ± epilepsy, autistic features, and attention deficit hyperactive disorder. Computational analysis of the missense variants suggest that the altered amino acid residues are likely to be located in protein regions important for function. This paper demonstrates that PRICKLE2 is involved in human neuronal development and that pathogenic variants in PRICKLE2 cause neurodevelopmental delay, behavioral difficulties and epilepsy in humans.
Author	Zweier, Christiane Bassuk, Alexander G. Rubboli, Guido Møller, Rikke S. Borredy, Kim Barcia, Guilia Kraus, Cornelia Bayat, Allan Iqbal, Sumaiya Weyhreter, Heike Amiel, Jeanne Chopra, Maya
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Cites_doi	10.1038/nmeth0410-248 10.1348/014466504772812940 10.1002/1097-4679(200012)56:12<1587::AID-9>3.0.CO;2-G 10.1038/mp.2013.71 10.1371/journal.pone.0080737 10.1002/da.20144 10.1016/j.pbiomolbio.2017.02.004 10.1002/humu.21589 10.1136/jnnp.41.2.140 10.1016/S0006-3223(00)00910-0 10.1016/j.ajhg.2016.01.009 10.1002/ajmg.a.40625 10.1016/S0092-8674(02)00715-8 10.1093/jb/mvr023 10.1002/humu.22844 10.1093/nar/gky1016 10.1016/j.pediatrneurol.2014.07.025 10.1002/gps.1989 10.1111/j.1528-1167.2009.02114.x 10.1016/0378-1119(88)90330-7 10.1097/YCT.0b013e318165c7b0 10.1016/j.ajhg.2008.10.003 10.1348/014466509X454868 10.1016/j.ajhg.2010.12.012
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Snippet	PRICKLE2 encodes a member of a highly conserved family of proteins that are involved in the non-canonical Wnt and planar cell polarity signaling pathway.... PRICKLE2 encodes a member of a highly conserved family of proteins that are involved in the non-canonical Wnt and planar cell polarity signaling pathway....
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SubjectTerms	Adolescent Adult Aged Amino acids Autism Child Codon, Nonsense Computational neuroscience Convulsions & seizures Developmental Disabilities - genetics Developmental Disabilities - pathology Epilepsy Female Frameshift Mutation Genetics Glutamic acid receptors (ionotropic) Hospitals Human subjects Humans LIM Domain Proteins - chemistry LIM Domain Proteins - genetics Male Membrane Proteins - chemistry Membrane Proteins - genetics Mutation, Missense N-Methyl-D-aspartic acid receptors Neurodevelopmental disorders Pathogenicity Pediatrics Phenotype Phenotypes Polarity Protein Domains Proteins Seizures Signal transduction Synaptic density Wnt protein
Title	PRICKLE2 revisited—further evidence implicating PRICKLE2 in neurodevelopmental disorders
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