Schaaf-Yang syndrome shows a Prader-Willi syndrome-like phenotype during infancy

Schaaf-Yang syndrome (SYS) is a newly recognized imprinting related syndrome, which is caused by a truncating variant in maternally imprinted MAGEL2 located in 15q11-q13. Yet, precise pathomechanism remains to be solved. We sequenced MAGEL2 in patients suspected Prader-Willi syndrome (PWS) to deline...

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Published inOrphanet journal of rare diseases Vol. 14; no. 1; p. 277
Main Authors Negishi, Yutaka, Ieda, Daisuke, Hori, Ikumi, Nozaki, Yasuyuki, Yamagata, Takanori, Komaki, Hirofumi, Tohyama, Jun, Nagasaki, Keisuke, Tada, Hiroko, Saitoh, Shinji
Format Journal Article
LanguageEnglish
Published England BioMed Central Ltd 02.12.2019
BioMed Central
BMC
Subjects
Amino acids
Arthrogryposis
Binding sites
Book publishing
Deoxyribonucleic acid
DNA
DNA methylation
DNA sequencing
Enzymes
Genes
Genetic aspects
Genomic imprinting
Genotype & phenotype
Growth hormones
Illnesses
Infants
Intellectual disabilities
MAGEL2
MAGEL2 gene
Medical research
Methylation
Neonates
Neurological deterioration
Newborn infants
Obesity
Patients
Phenotypes
Prader-Willi syndrome
Rare diseases
Schaaf-Yang syndrome
Siblings
United States > US
MAGEL2
Neurological deterioration
Schaaf-Yang syndrome
Genomic imprinting
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Summary:Schaaf-Yang syndrome (SYS) is a newly recognized imprinting related syndrome, which is caused by a truncating variant in maternally imprinted MAGEL2 located in 15q11-q13. Yet, precise pathomechanism remains to be solved. We sequenced MAGEL2 in patients suspected Prader-Willi syndrome (PWS) to delineate clinical presentation of SYS. We examined 105 patients with clinically suspected PWS but without a specific PWS genetic alteration. Sanger sequencing of the entire MAGEL2 gene and methylation-specific restriction enzyme treatment to detect the parent of origin were performed. Clinical presentation was retrospectively assessed in detail. Truncating variants in MAGEL2 were detected in six patients (5.7%), including a pair of siblings. All truncating variants in affected patients were on the paternally derived chromosome, while the healthy father of the affected siblings inherited the variant from his mother. Patients with MAGEL2 variants shared several features with PWS, such as neonatal hypotonia, poor suck, and obesity; however, there were also unique features, including arthrogryposis and a failure to acquire meaningful words. Additionally, an episode of neurological deterioration following febrile illness was confirmed in four of the six patients, which caused severe neurological sequalae. SYS can be present in infants suspected with PWS but some unique features, such as arthrogryposis, can help discriminate between the two syndromes. An episode of neurological deterioration following febrile illness should be recognized as an important complication.
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ISSN:1750-1172
1750-1172
DOI:10.1186/s13023-019-1249-4