Sleep disturbances in Phelan‐McDermid syndrome: Clinical and metabolic profiling of 56 individuals

Phelan‐McDermid Syndrome (PMS) is caused by deletions at chromosome 22q13.3 or pathogenic/likely pathogenic SHANK3 variants. The clinical presentation is extremely variable and includes global developmental delay/intellectual disability (ID), seizures, neonatal hypotonia, and sleep disturbances, amo...

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Published in	Clinical genetics Vol. 104; no. 2; pp. 198 - 209
Main Authors	Moffitt, Bridgette A., Oberman, Lindsay M., Beamer, Laura, Srikanth, Sujata, Jain, Lavanya, Cascio, Lauren, Jones, Kelly, Pauly, Rini, May, Melanie, Skinner, Cindy, Buchanan, Caroline, DuPont, Barbara R., Kaufmann, Walter E., Valentine, Kathleen, Ward, Linda D., Ivankovic, Diana, Rogers, R. Curtis, Phelan, Katy, Sarasua, Sara M., Boccuto, Luigi
Format	Journal Article
Language	English
Published	Oxford, UK Blackwell Publishing Ltd 01.08.2023
Subjects	22q13 deletion syndrome Animals Chromosome 22 Chromosome Deletion Chromosome Disorders - genetics Chromosomes, Human, Pair 22 - genetics DNA microarrays Humans Intellectual disabilities Mammals - genetics Metabolism Neonates Phelan‐McDermid syndrome Phenotype Phenotypes PMS Seizures SHANK3 Sleep Sleep - genetics sleep disturbance Sleep Wake Disorders - complications Sleep Wake Disorders - genetics Phelan-McDermid syndrome sleep disturbance SHANK3 PMS 22q13 deletion syndrome
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Abstract	Phelan‐McDermid Syndrome (PMS) is caused by deletions at chromosome 22q13.3 or pathogenic/likely pathogenic SHANK3 variants. The clinical presentation is extremely variable and includes global developmental delay/intellectual disability (ID), seizures, neonatal hypotonia, and sleep disturbances, among others. This study investigated the prevalence of sleep disturbances, and the genetic and metabolic features associated with them, in a cohort of 56 individuals with PMS. Sleep data were collected via standardized observer/caregiver questionnaires, while genetic data from array‐CGH and sequencing of 9 candidate genes within the 22q13.3 region, and metabolic profiling utilized the Biolog Phenotype Mammalian MicroArray plates. Sleep disturbances were present in 64.3% of individuals with PMS, with the most common problem being waking during the night (39%). Sleep disturbances were more prevalent in individuals with a SHANK3 pathogenic variant (89%) compared to subjects with 22q13.3 deletions of any size (59.6%). Distinct metabolic profiles for individuals with PMS with and without sleep disturbances were also identified. These data are helpful information for recognizing and managing sleep disturbances in individuals with PMS, outlining the main candidate gene for this neurological manifestation, and highlighting potential biomarkers for early identification of at‐risk subjects and molecular targets for novel treatment approaches.
AbstractList	Phelan‐McDermid Syndrome (PMS) is caused by deletions at chromosome 22q13.3 or pathogenic/likely pathogenic SHANK3 variants. The clinical presentation is extremely variable and includes global developmental delay/intellectual disability (ID), seizures, neonatal hypotonia, and sleep disturbances, among others. This study investigated the prevalence of sleep disturbances, and the genetic and metabolic features associated with them, in a cohort of 56 individuals with PMS. Sleep data were collected via standardized observer/caregiver questionnaires, while genetic data from array‐CGH and sequencing of 9 candidate genes within the 22q13.3 region, and metabolic profiling utilized the Biolog Phenotype Mammalian MicroArray plates. Sleep disturbances were present in 64.3% of individuals with PMS, with the most common problem being waking during the night (39%). Sleep disturbances were more prevalent in individuals with a SHANK3 pathogenic variant (89%) compared to subjects with 22q13.3 deletions of any size (59.6%). Distinct metabolic profiles for individuals with PMS with and without sleep disturbances were also identified. These data are helpful information for recognizing and managing sleep disturbances in individuals with PMS, outlining the main candidate gene for this neurological manifestation, and highlighting potential biomarkers for early identification of at‐risk subjects and molecular targets for novel treatment approaches. Phelan‐McDermid Syndrome (PMS) is caused by deletions at chromosome 22q13.3 or pathogenic/likely pathogenic SHANK3 variants. The clinical presentation is extremely variable and includes global developmental delay/intellectual disability (ID), seizures, neonatal hypotonia, and sleep disturbances, among others. This study investigated the prevalence of sleep disturbances, and the genetic and metabolic features associated with them, in a cohort of 56 individuals with PMS. Sleep data were collected via standardized observer/caregiver questionnaires, while genetic data from array‐CGH and sequencing of 9 candidate genes within the 22q13.3 region, and metabolic profiling utilized the Biolog Phenotype Mammalian MicroArray plates. Sleep disturbances were present in 64.3% of individuals with PMS, with the most common problem being waking during the night (39%). Sleep disturbances were more prevalent in individuals with a SHANK3 pathogenic variant (89%) compared to subjects with 22q13.3 deletions of any size (59.6%). Distinct metabolic profiles for individuals with PMS with and without sleep disturbances were also identified. These data are helpful information for recognizing and managing sleep disturbances in individuals with PMS, outlining the main candidate gene for this neurological manifestation, and highlighting potential biomarkers for early identification of at‐risk subjects and molecular targets for novel treatment approaches. Phelan-McDermid Syndrome (PMS) is caused by deletions at chromosome 22q13.3 or pathogenic/likely pathogenic SHANK3 variants. The clinical presentation is extremely variable and includes global developmental delay/intellectual disability (ID), seizures, neonatal hypotonia, and sleep disturbances, among others. This study investigated the prevalence of sleep disturbances, and the genetic and metabolic features associated with them, in a cohort of 56 individuals with PMS. Sleep data were collected via standardized observer/caregiver questionnaires, while genetic data from array-CGH and sequencing of 9 candidate genes within the 22q13.3 region, and metabolic profiling utilized the Biolog Phenotype Mammalian MicroArray plates. Sleep disturbances were present in 64.3% of individuals with PMS, with the most common problem being waking during the night (39%). Sleep disturbances were more prevalent in individuals with a SHANK3 pathogenic variant (89%) compared to subjects with 22q13.3 deletions of any size (59.6%). Distinct metabolic profiles for individuals with PMS with and without sleep disturbances were also identified. These data are helpful information for recognizing and managing sleep disturbances in individuals with PMS, outlining the main candidate gene for this neurological manifestation, and highlighting potential biomarkers for early identification of at-risk subjects and molecular targets for novel treatment approaches.Phelan-McDermid Syndrome (PMS) is caused by deletions at chromosome 22q13.3 or pathogenic/likely pathogenic SHANK3 variants. The clinical presentation is extremely variable and includes global developmental delay/intellectual disability (ID), seizures, neonatal hypotonia, and sleep disturbances, among others. This study investigated the prevalence of sleep disturbances, and the genetic and metabolic features associated with them, in a cohort of 56 individuals with PMS. Sleep data were collected via standardized observer/caregiver questionnaires, while genetic data from array-CGH and sequencing of 9 candidate genes within the 22q13.3 region, and metabolic profiling utilized the Biolog Phenotype Mammalian MicroArray plates. Sleep disturbances were present in 64.3% of individuals with PMS, with the most common problem being waking during the night (39%). Sleep disturbances were more prevalent in individuals with a SHANK3 pathogenic variant (89%) compared to subjects with 22q13.3 deletions of any size (59.6%). Distinct metabolic profiles for individuals with PMS with and without sleep disturbances were also identified. These data are helpful information for recognizing and managing sleep disturbances in individuals with PMS, outlining the main candidate gene for this neurological manifestation, and highlighting potential biomarkers for early identification of at-risk subjects and molecular targets for novel treatment approaches.
Author	DuPont, Barbara R. Boccuto, Luigi Jones, Kelly Ward, Linda D. Phelan, Katy Beamer, Laura Rogers, R. Curtis Jain, Lavanya May, Melanie Kaufmann, Walter E. Sarasua, Sara M. Buchanan, Caroline Oberman, Lindsay M. Pauly, Rini Cascio, Lauren Srikanth, Sujata Valentine, Kathleen Skinner, Cindy Moffitt, Bridgette A. Ivankovic, Diana
AuthorAffiliation	3 Greenwood Genetic Center, Greenwood, SC 29646, USA 8 Genetics Department, Florida Cancer Specialists & Research Institute, Fort Myers, Florida, USA 6 Department of Neurology, Boston Children's Hospital, Boston, Massachusetts, USA 7 Anavex Life Sciences Corp, New York, New York, USA 2 Noninvasive Neuromodulation Unit, Experimental Therapeutics and Pathophysiology Branch, National Institute of Mental Health, National Institutes of Health, Bethesda, Maryland 20892, USA 5 Department of Human Genetics, Emory University School of Medicine, Atlanta, Georgia, USA 1 School of Nursing, Healthcare Genetics Program, Clemson University, Clemson, South Carolina 29634, USA 4 Genomic Medicine Institute, Cleveland Clinic, Cleveland, Ohio 44195
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Copyright	2023 The Authors. published by John Wiley & Sons Ltd. 2023 The Authors. Clinical Genetics published by John Wiley & Sons Ltd. 2023. This article is published under http://creativecommons.org/licenses/by-nc-nd/4.0/ (the “License”). Notwithstanding the ProQuest Terms and Conditions, you may use this content in accordance with the terms of the License.
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Keywords	Phelan-McDermid syndrome sleep disturbance SHANK3 PMS 22q13 deletion syndrome
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Notes	ObjectType-Article-1 SourceType-Scholarly Journals-1 ObjectType-Feature-2 content type line 14 content type line 23 Author Contributions BAM wrote and submitted the manuscript. BAM, LB, and SMS formulated the paper and created the research design. LMO and L. Beamer collected clinical data from patients. LJ, SS, CK, KJ, MM, LC, and BD transformed blood samples into LCLs, collected Biolog data, and sequenced available patient samples. RCR, KP, WEK, SMS, and LB reviewed the manuscript. All authors have read and agreed to the published version of the manuscript.
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Snippet	Phelan‐McDermid Syndrome (PMS) is caused by deletions at chromosome 22q13.3 or pathogenic/likely pathogenic SHANK3 variants. The clinical presentation is... Phelan‐McDermid Syndrome (PMS) is caused by deletions at chromosome 22q13.3 or pathogenic/likely pathogenic SHANK3 variants. The clinical presentation is... Phelan-McDermid Syndrome (PMS) is caused by deletions at chromosome 22q13.3 or pathogenic/likely pathogenic SHANK3 variants. The clinical presentation is... Phelan-McDermid Syndrome (PMS) is caused by deletions at chromosome 22q13.3 or pathogenic/likely pathogenic SHANK3 variants. The clinical presentation is...
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SubjectTerms	22q13 deletion syndrome Animals Chromosome 22 Chromosome Deletion Chromosome Disorders - genetics Chromosomes, Human, Pair 22 - genetics DNA microarrays Humans Intellectual disabilities Mammals - genetics Metabolism Neonates Phelan‐McDermid syndrome Phenotype Phenotypes PMS Seizures SHANK3 Sleep Sleep - genetics sleep disturbance Sleep Wake Disorders - complications Sleep Wake Disorders - genetics
Title	Sleep disturbances in Phelan‐McDermid syndrome: Clinical and metabolic profiling of 56 individuals
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