Multi-disciplinary clinical study of Smith-Magenis syndrome (deletion 17p11.2)

Greenberg, Frank; Lewis, Richard A.; Potocki, Lorraine; Glaze, Daniel G.; Parke, Julie T.; Killian, James M.; Murphy, Mary; Williamson, Dominic J.; Brown, Frank R.; Dutton, Robert V.; McCluggage, Charles W.; Friedman, Ellen M.; Sulek, Marcelle; Lupski, James R.

doi:10.1002/(sici)1096-8628(19960329)62:3<247::aid-ajmg9>3.0.co;2-q

Cited by 290 publications

(202 citation statements)

References 34 publications

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“…Patients with the apparent reciprocal duplication of the WBS region have mild dysmorphisms and a severe delay in expressive language 46 47 48. In most cases, the increased dosage from duplication causes a milder phenotype than deletion of the same region as in the Smith–Magenis syndrome (SMS, MIM 182290) and its reciprocal duplication syndrome, Potocki–Lupski syndrome (PTLS, MIM 610883),49 50 as well as in the duplication and loss of function of the MECP2 gene 51 52 53. Patients with SMS have characteristic craniofacial, skeletal and neurobehavioral features as well as defects in multiple organ systems.…”

Section: Discussionmentioning

confidence: 99%

Genomic duplication resulting in increased copy number of genes encoding the sister chromatid cohesion complex conveys clinical consequences distinct from Cornelia de Lange

Yan

Zhang

Brundage

et al. 2008

Journal of Medical Genetics

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Cornelia de Lange Syndrome (CdLS) is a multisystem congenital anomaly disorder. Heterozygous point mutations in three genes (NIPBL, SMC3 and SMC1A), encoding components of the sister chromatid cohesion apparatus, are responsible for ∼ 50-60% of CdLS cases. Recent studies have revealed a high degree of genomic rearrangements (e.g. deletions and duplications) in the human genome, which result in gene copy number variations (CNV). CNVs have been associated with a wide range of both Mendelian and complex traits including disease phenotypes such as Charcot-Marie-Tooth type 1A, Pelizaeus-Merzbacher, Parkinson, Alzheimer, autism and schizophrenia. Increased versus decreased copy number of the same gene can potentially cause either similar or different clinical features. We identified duplications on chromosomes 5 or X using genome wide array Comparative Genomic Hybridization (aCGH). The duplicated regions contain either the NIPBL or the SMC1A genes. Junction sequences analyses revealed the involvement of three genomic rearrangement mechanisms. The patients share some common features including mental retardation, developmental delay, sleep abnormalities, and crainofacial and limb defects. The systems affected are the same as in CdLS, but clinical manifestations are distinct from CdLS; particularly the absence of the CdLS facial gestalt. Our results confirm the notion that duplication CNV of genes can be a common mechanism for human genetic diseases. Defining the clinical consequences for a specific gene dosage alteration represents a new “reverse genomics” trend in medical genetics that is reciprocal to the traditional approach of delineation of the common clinical phenotype preceding the discovery of the genetic etiology.

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Section: Discussionmentioning

confidence: 99%

Genomic duplication resulting in increased copy number of genes encoding the sister chromatid cohesion complex conveys clinical consequences distinct from Cornelia de Lange

Yan

Zhang

Brundage

et al. 2008

Journal of Medical Genetics

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“…A prominent CNV disorder is Smith-Magenis syndrome (SMS) (Smith et al, 1986), which affects one in ~15,000 individuals. SMS patients exhibit craniofacial abnormalities, obesity, circadian abnormality, hypotonia, intellectual disabilities, stereotypies, and autistic features (Greenberg et al, 1996; Smith et al, 1993). 70% of SMS patients have a ~3.7 Mb interstitial deletion of chromosome 17p11.2 that contains 76 genes (Elsea and Girirajan, 2008).…”

Section: Introductionmentioning

confidence: 99%

Molecular and Neural Functions of Rai1 , the Causal Gene for Smith-Magenis Syndrome

Huang

Guenthner

et al. 2016

Neuron

110

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SUMMARY Haploinsufficiency of Retinoic Acid Induced 1 (RAI1) causes Smith-Magenis syndrome (SMS), which is associated with diverse neurodevelopmental and behavioral symptoms as well as obesity. RAI1 encodes a nuclear protein but little is known about its molecular function or the cell types responsible for SMS symptoms. Using genetically engineered mice, we found that Rai1 preferentially occupies DNA regions near active promoters and promotes the expression of a group of genes involved in circuit assembly and neuronal communication. Behavioral analyses demonstrated that pan-neural loss of Rai1 causes deficits in motor function, learning, and food intake. These SMS-like phenotypes are produced by loss of Rai1 function in distinct neuronal types: Rai1 loss in inhibitory neurons or subcortical glutamatergic neurons causes learning deficits, while Rai1 loss in Sim1+ or SF1+ cells causes obesity. By integrating molecular and organismal analyses, our study suggests potential therapeutic avenues for a complex neurodevelopmental disorder.

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“…The sleep abnormalities include daytime sleepiness, difficulty falling asleep at night, nocturnal awakening, decreased sleep time, and abnormalities in the percentage of rapid eye movement (REM) sleep 67 We have previously reported abnormalities in REM sleep in SMS 6. In this report an additional cohort of SMS patients was studied more extensively to define the spectrum of sleep abnormalities further.…”

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confidence: 95%

Circadian rhythm abnormalities of melatonin in Smith-Magenis syndrome

Potocki

2000

Journal of Medical Genetics

177

165

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Background-Smith-Magenis syndrome (SMS) is a multiple congenital anomalies/ mental retardation syndrome associated with a hemizygous deletion of chromosome 17, band p11.2. Characteristic features include neurobehavioural abnormalities such as aggressive and self-injurious behaviour and significant sleep disturbances. The majority of patients have a common deletion characterised at the molecular level. Physical mapping studies indicate that all patients with the common deletion are haploinsuYcient for subunit 3 of the COP9 signalosome (COPS3), which is conserved from plants to humans, and in the plant Arabidopis thaliana regulates gene transcription in response to light. HaploinsuYciency of this gene is hypothesised to be potentially involved in the sleep disturbances seen in these patients. Melatonin is a hormone secreted by the pineal gland. SMS patients are reported to have fewer sleep disturbances when given a night time dose of this sleep inducing hormone. Methods-Urinary excretion of 6-sulphatoxymelatonin (aMT6s), the major hepatic metabolite of melatonin, in 19 SMS patients were measured in conjunction with 24 hour sleep studies in 28 SMS patients. Five of the 28 patients did not have the common SMS deletion. To investigate a potential correlation of COPS3 haploinsufficiency and disturbed melatonin excretion, we performed fluorescence in situ hybridisation (FISH) using two BACs containing coding exons of COPS3. Results-All SMS patients show significant sleep disturbances when assessed by objective criteria. Abnormalities in the circadian rhythm of aMT6s were observed in all but one SMS patient. Interestingly this patient did not have the common deletion. All patients studied, including the one patient with a normal melatonin rhythm, were haploinsuYcient for COPS3. Conclusions-Our data indicate a disturbed circadian rhythm in melatonin and document the disturbed sleep pattern in Smith-Magenis syndrome. Our findings suggest that the abnormalities in the circadian rhythm of melatonin and altered sleep patterns could be secondary to aberrations in the production, secretion, distribution, or metabolism of melatonin; however, a direct role for COPS3 could not be established. (J Med Genet 2000;37:428-433)

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Multi-disciplinary clinical study of Smith-Magenis syndrome (deletion 17p11.2)

Cited by 290 publications

References 34 publications

Genomic duplication resulting in increased copy number of genes encoding the sister chromatid cohesion complex conveys clinical consequences distinct from Cornelia de Lange

Genomic duplication resulting in increased copy number of genes encoding the sister chromatid cohesion complex conveys clinical consequences distinct from Cornelia de Lange

Molecular and Neural Functions of Rai1 , the Causal Gene for Smith-Magenis Syndrome

Circadian rhythm abnormalities of melatonin in Smith-Magenis syndrome

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