Truncating mutations of MAGEL2 cause Prader-Willi phenotypes and autism.

paper Cited Public

Authors: Schaaf, Christian P; Gonzalez-Garay, Manuel L; Xia, Fan; Potocki, Lorraine; Gripp, Karen W; Zhang, Baili; Peters, Brock A; McElwain, Mark A; Drmanac, Radoje; Beaudet, Arthur L; Caskey, C Thomas; Yang, Yaping
Year: 2013
Journal: Nature genetics
PMID: 24076603
DOI: 10.1038/ng.2776
PMCID: PMC3819162

#	Section	Preview
0	Online Methods — Human subjects	Patient 1 and his parents were enrolled in a whole genome sequencing study, approved by the…
1	Online Methods — Human subjects	Following the identification of truncating MAGEL2 mutations, Patients 2–4 and their respective…
2	Online Methods — Whole genome sequencing analysis	Family 1 comprises two healthy parents and an affected son. Their DNA was sent to Complete Genomics,…
3	Online Methods — Phasing de novo mutation in MAGEL2 (also see Supplementary Figure 2)	Patient 1’s purified DNA was aliquoted at ~0.1 genome equivalents per well across a 384-well plate…
4	Online Methods — Phasing de novo mutation in MAGEL2 (also see Supplementary Figure 2)	After heat inactivation of the MDA reaction, each well was diluted 13.4-fold with water. An aliquot…
5	Online Methods — Phasing de novo mutation in MAGEL2 (also see Supplementary Figure 2)	Wells in which SNP regions were amplified by qPCR were assumed to contain DNA fragments spanning the…
6	Online Methods — Phasing de novo mutation in MAGEL2 (also see Supplementary Figure 2)	KAPA HiFi and Pfu PCR products were gel purified (GeneJET Gel Extraction Kit, Fermentas, Waltham,…
7	Online Methods — Copy number variation and methylation	We verified the absence of any copy number variation in the PWS region (15q11.2-q13) by analysis of…
8	Online Methods — Methylations-sensitive digestion of MAGEL2 followed by Sanger sequencing	Patient DNA was digested with restriction endonuclease SmaI (New England Biosystems, Ipswich, MA,…

Name	Type
15q11.2-q13 local	variant
Affected_Son local	phenotype
autism spectrum disorder	phenotype
clinical whole exome sequencing local	cohort
de novo variant	variant
developmental delay	phenotype
Elim Biopharmaceuticals local	drug
Family_1 local	cohort
Fermentas local	drug
GeneJET Gel Extraction Kit local	drug
intellectual disability	phenotype
KAPA HiFi local	drug
KAPA HiFi HotStart ReadyMix local	drug
MAGEL2	gene
MAGEL2_p.Ala551fs local	variant
MDA product local	drug
mSNP-422 local	variant
mSNP-506 local	variant
mSNP+8032 local	variant
MYO1H local	gene
MYO1H_Ala83Val local	variant
parents	cohort
Patient 1 local	cohort
Patients 2–4 local	cohort
Pfu local	drug
PfuTurboCx polymerase local	drug
Prader-Willi syndrome	phenotype
pSNP-12785 local	variant
referred subjects local	cohort
SmaI	drug
SNP	cohort
SYBR Green Master Mix local	drug
truncating MAGEL2 mutation local	variant
uracil-N-glycosylase	drug
UTP local	drug
whole genome sequencing study local	cohort

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In this knowledge base

Title	Year	PMID
Parent-of-origin-specific allelic associations among 106 genomic loci for age at menarche.	2014	25231870

External

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Targeting the histone methyltransferase G9a activates imprinted genes and improves survival of a mouse model of Prader-Willi syndrome.	Kim Y et al.	—	2017	→
The phenotypic spectrum of Schaaf-Yang syndrome: 18 new affected individuals from 14 families.	Fountain MD et al.	—	2017	→
The Prader-Willi syndrome proteins MAGEL2 and necdin regulate leptin receptor cell surface abundance through ubiquitination pathways.	Wijesuriya TM et al.	—	2017	→
The Use of Oxytocin to Improve Feeding and Social Skills in Infants With Prader-Willi Syndrome.	Tauber M et al.	—	2017	→
Analysis of Genome-Wide Monoallelic Expression Patterns in Three Major Cell Types of Mouse Visual Cortex Using Laser Capture Microdissection.	Lin CY et al.	—	2016	→
Clinical and Neurobiological Relevance of Current Animal Models of Autism Spectrum Disorders.	Kim KC et al.	—	2016	→
Coexpression profiles reveal hidden gene networks.	Chachlaki K et al.	—	2016	→
DNA methylation analysis in constitutional disorders: Clinical implications of the epigenome.	Schenkel LC et al.	—	2016	→
Dyssynchrony and perinatal psychopathology impact of child disease on parents-child interactions, the paradigm of Prader Willi syndrom.	Viaux-Savelon S et al.	—	2016	→
Endosomal system genetics and autism spectrum disorders: A literature review.	Patak J et al.	—	2016	→
Epigenetic alterations induced by environmental stress associated with metabolic and neurodevelopmental disorders.	Kubota T	—	2016	→
Epigenetic Effect of Environmental Factors on Autism Spectrum Disorders.	Kubota T et al.	—	2016	→
Epigenetics and Human Disease.	Zoghbi HY et al.	—	2016	→
Forebrain neurogenesis: From embryo to adult.	Dennis D et al.	—	2016	→
Genes with high penetrance for syndromic and non-syndromic autism typically function within the nucleus and regulate gene expression.	Casanova EL et al.	—	2016	→
Genetics of Prader-Willi syndrome and Prader-Will-Like syndrome.	Cheon CK	—	2016	→
Imprinting: the Achilles heel of trio-based exome sequencing.	Aten E et al.	—	2016	→
Magel2-null mice are hyper-responsive to setmelanotide, a melanocortin 4 receptor agonist.	Bischof JM et al.	—	2016	→
Muscle dysfunction caused by loss of Magel2 in a mouse model of Prader-Willi and Schaaf-Yang syndromes.	Kamaludin AA et al.	—	2016	→
New Perspectives on Genomic Imprinting, an Essential and Multifaceted Mode of Epigenetic Control in the Developing and Adult Brain.	Perez JD et al.	—	2016	→
Prader-Willi Syndrome and Schaaf-Yang Syndrome: Neurodevelopmental Diseases Intersecting at the <i>MAGEL2</i> Gene.	Fountain MD et al.	—	2016	→
Prader-Willi Syndrome: The Disease that Opened up Epigenomic-Based Preemptive Medicine.	Kubota T et al.	—	2016	→
Rare Genetic Forms of Obesity: Clinical Approach and Current Treatments in 2016.	Huvenne H et al.	—	2016	→
Rare Syndromes and Common Variants of the Brain-Derived Neurotrophic Factor Gene in Human Obesity.	Han JC	—	2016	→
Single Gene and Syndromic Causes of Obesity: Illustrative Examples.	Butler MG	—	2016	→
Sleeve gastrectomy leads to weight loss in the Magel2 knockout mouse.	Arble DM et al.	—	2016	→
Tandem repeat knockout utilizing the CRISPR/Cas9 system in human cells.	Lv Q et al.	—	2016	→
The genetics of pubertal timing in the general population: recent advances and evidence for sex-specificity.	Cousminer DL et al.	—	2016	→
Unifying Views of Autism Spectrum Disorders: A Consideration of Autoregulatory Feedback Loops.	Mullins C et al.	—	2016	→
An Early Postnatal Oxytocin Treatment Prevents Social and Learning Deficits in Adult Mice Deficient for Magel2, a Gene Involved in Prader-Willi Syndrome and Autism.	Meziane H et al.	—	2015	→
Angelman syndrome imprinting center encodes a transcriptional promoter.	Lewis MW et al.	—	2015	→
Coding and noncoding expression patterns associated with rare obesity-related disorders: Prader-Willi and Alström syndromes.	Butler MG et al.	—	2015	→
Detection and phasing of single base de novo mutations in biopsies from human in vitro fertilized embryos by advanced whole-genome sequencing.	Peters BA et al.	—	2015	→
Discovery of Rare Mutations in Autism: Elucidating Neurodevelopmental Mechanisms.	Gamsiz ED et al.	—	2015	→
Genomic conflicts and sexual antagonism in human health: insights from oxytocin and testosterone.	Mokkonen M et al.	—	2015	→
Haplotype-resolved genome sequencing: experimental methods and applications.	Snyder MW et al.	—	2015	→
Highly restricted deletion of the SNORD116 region is implicated in Prader-Willi Syndrome.	Bieth E et al.	—	2015	→
MAGEL2 and Oxytocin-Implications in Prader-Willi Syndrome and Beyond.	Fountain MD et al.	—	2015	→
Model mice for 15q11-13 duplication syndrome exhibit late-onset obesity and altered lipid metabolism.	Kishimoto R et al.	—	2015	→
Plasma metabolomic profiles enhance precision medicine for volunteers of normal health.	Guo L et al.	—	2015	→
Prader-Willi syndrome: a review of clinical, genetic, and endocrine findings.	Angulo MA et al.	—	2015	→
Progressive postnatal decline in leptin sensitivity of arcuate hypothalamic neurons in the Magel2-null mouse model of Prader-Willi syndrome.	Pravdivyi I et al.	—	2015	→
Truncating Homozygous Mutation of Carboxypeptidase E (CPE) in a Morbidly Obese Female with Type 2 Diabetes Mellitus, Intellectual Disability and Hypogonadotrophic Hypogonadism.	Alsters SI et al.	—	2015	→
Truncating Mutations of MAGEL2, a Gene within the Prader-Willi Locus, Are Responsible for Severe Arthrogryposis.	Mejlachowicz D et al.	—	2015	→
USP7 Acts as a Molecular Rheostat to Promote WASH-Dependent Endosomal Protein Recycling and Is Mutated in a Human Neurodevelopmental Disorder.	Hao YH et al.	—	2015	→
Advances in Genetic Discovery and Implications for Counseling of Patients and Families with Autism Spectrum Disorders.	Shen J et al.	—	2014	→
[Beyond usual functions of snoRNAs].	Abel Y et al.	—	2014	→
Clinical phenotypes of MAGEL2 mutations and deletions.	Buiting K et al.	—	2014	→
Co-barcoded sequence reads from long DNA fragments: a cost-effective solution for "perfect genome" sequencing.	Peters BA et al.	—	2014	→
Effectiveness of exome and genome sequencing guided by acuity of illness for diagnosis of neurodevelopmental disorders.	Soden SE et al.	—	2014	→
Ontogenesis of oxytocin pathways in the mammalian brain: late maturation and psychosocial disorders.	Grinevich V et al.	—	2014	→
Parent-of-origin-specific allelic associations among 106 genomic loci for age at menarche.	Perry JR et al.	—	2014	→
Reactivation of maternal SNORD116 cluster via SETDB1 knockdown in Prader-Willi syndrome iPSCs.	Cruvinel E et al.	—	2014	→
The role of genomic imprinting in biology and disease: an expanding view.	Peters J	—	2014	→
Natural breaking of the maternal silence at the mouse and human imprinted Prader-Willi locus: A whisper with functional consequences.	Matarazzo V et al.	—	2013	→
Personalized genomic disease risk of volunteers.	Gonzalez-Garay ML et al.	—	2013	→