Angelman syndrome: Difference between revisions

Editor-In-Chief: C. Michael Gibson, M.S., M.D. [1]; Associate Editor(s)-in-Chief: Moises Romo, M.D.

Overview

Angelman syndrome, formerly known as "happy puppet syndrome", is a genetic disorder characterized by intelectual and development delay, seizures, puppet-like movement, unprovoked laughter/smiling, and excessive socialization with strangers.

Historical Perspective

• Angelman syndrome was first discovered by Dr. Harry Angelman, a British pediatrician, in 1965 during his seminar, where he described three children with the typical facies of the syndrome.^[1][2]
• In 1965,Dr. Angelman quoted in his seminal paper:

"I happened to see an oil painting...called... "a Boy with a Puppet". The boy's laughing face and the fact that my patients exhibited jerky movements gave me the idea of writing an article about the three children with a title of Puppet Children."^[1]

• In 1987, maternal allele deletion in chromosome 15 was first identified in the pathogenesis of Angelman syndrome.^[3]
• In 1994 point mutations in UBE3A gene was known to be the gene responsible for Angelman syndrome.^[3][4]

Pathophysiology

Modes of Inheritance

• In 70% of the cases, Angelman syndrome is caused by a sporadic (de novo) maternal deletion in chromosomal region 15q11-13 causing an absence of UBE3A gene, involving the ubiquitin pathway.^[5][6][7] There is a lack of expression of the maternally-inherited UBE3A gene in the brain, while the paternally-inherited copy of UBE3A is silenced.^[8]
• Other causes include paternal uniparental disomy, impringting error, translocation, or single gene mutation in UBE3A.^[9][7]
• 3-5% of cases of Angelman syndrome can be inherited.^[10][11]
• Recurrence of Angelman syndrome in subsequent children when having a child with a de novo deletion is estimated around 1%.^[12]
• In approximately 10% of cases, no cause can be identified.^[10]

Phenotype-Gene Relationships

Clinical Features

Angelman syndrome is characterized by:

• Puppet-like movement^{[13][14][7][15]}
• Intelectual and development delay^{[13][16][7][15]}
• Seizures^[13][7][15]
• Unprovoked laughter/smiling^[13][14]
• Excessive socialization with strangers^[13]
• Speech impairment^[14][7][15]

Other less common features are:

• Delayed head circumference growth^[17]

• Suck/swallowing disorders^[17][15]
• Feeding problems^[17]
• Frequent drooling^[17]
• Excessive chewing^[17]
• Wide based gait^[17][14]
• Increased sensitivity to heat^[17]
• Diminished need for sleep^[17]
• Hydrophilia^[17]
• Fascination with crinkly things^[17]
• Abnormal feeding conducts^[17]
• Constipation^[17]

Differentiating Angelman syndrome from Other Diseases

Angelman syndrome must be differentiated from other diseases that cause intelectual and development delay, dysmorphic facies, and seizures, such as:

Epidemiology and Demographics

• The prevalence of Angelman syndrome is approximately 5-7 per 100,000 individuals worldwide.^[18]
• The exact incidence of Angelman syndrome is unknown, but its estimated to be between 6-7 per 100,000 births .^[19]

Age

Full spectrum of the disease appears usually before 3 years of age.^[20]

Gender

Angelman syndrome affects men and women equally.^[18][21]

Race

There is no racial predilection for Angelman syndrome.^[22]

Risk Factors

There are no risk factors for developing Angelman syndrome, since most of the cases occur due to a de novo deletion and there is a very small chance for this condition to be hereditary transmitted.^[23]

Screening

Prenatal screening of 15q11.2-q13 region mutations is possible through DNA and/or chromosomal/FISH analysis of fetal cells acquired by chorionic villus sampling or amniocentesis.^[15]

Screening for Angelman syndrome-suspected patients can be made by the following tests:

• Karyotyping. Is warranted for any patient with suspected Angelman syndrome.^[24]
• Fluorescent in situ hybridization (FISH). May detect deletions, but not imprinting centers or uniparental disomy.^[24]
• Methylation test. May detect deletions, uniparental disomies, and imprinting mutations, but not UBE3A gene mutation.^[24]
• Paternal uniparental disomy (UPD) studies. Usually done after a normal FISH and methylation test.^[24]
• Ubiquitin-protein ligase E3A (UBE3A) mutations. Is performed in patients with clinical presentation of Angelman syndrome, but negative methylation test.^[24]
• Imprinting center (IC) mutations. Detects small deletions, but is only available in research centers.^[24]

Natural History, Complications & Prognosis

• Newborns with Angelman syndrome usually weight less than averange when delivered.^[25]
• Motor delay and jerky movements usually appear before 1 year of age.^[25][7]
• Seizures could be present between 2 and 8 years of age.^[25][7]
• Dysmorphic facies and scoliosis are aparent after 5 years of age.^{[25][26][27][7]}
• Sexual developement begins and progresses at a normal time.^[28][29]
• Dressing skills and use of certain utensils may happen.^[26]
• Patients never develope proper language (5-10 learned word) and usually comunicate with signs.^[25][7][30]
• At the end, patients do not acquire enough abilities to live by there own.^[25]
• Prognosis will vary depending on the severity of symptoms and earliness of management.^[31]
• Patients may have a normal life span.^[31]
• The mortality rate of Angelman syndrome per 1000 patients/year was 15.84.^[32]

Diagnosis

Diagnostic Criteria

The Angelman Syndrome Foundation defined criteria for diagnosis in 1995, and updated his criteria in 2006.^[33]

The diagnosis of Angelman syndrome according to the Scientific Advisory Committee of the US Angelman syndrome Foundation (Williams et al 2006) is based on:^[34][35][36]

• Developement history. Normal birth, delayed motor milestones, with no loss of skills.^[35][7]
• Clinical findings. Clinical features (puppet-like movements, speech impairment, feeding dificulties, unprovoked laughter, etc.) previously described, dysmorphic facies, and behavioural uniqueness.^[35]
• Genetic testing. Deletion in chromosomal region 15q11-13 with absence of UBE3A gene.^[35]

Symptoms

Angelman syndrome is usually asymptomatic.

Physical Examination

• Patients with Angelman syndrome usually appear dysmorphic.^[37][15]
• The most common physical examination findings are:^[35]

• Flat occiput ^[17]
• Below average head size^[38][15]
• Occipital groove^[17]
• Protruding tongue^[17][15]
• Tongue thrusting^[17]
• Truncal hypotonia^[17]
• Prognathia^[17]
• Wide mouth^[17]
• Wide spaced teeth^[17]
• Strabismus^[17]
• Light color of skin,hair, and eyes^[17]
• Uplifted, flexed arm position during ambulation^[17]
• Valgus positioned ankles^[17]
• Obesity found in older child^[17]
• Scoliosis^[17][15]

Laboratory Findings

• Hematologic, metabolic, and chemical laboratory findings in Angelman syndrome are usually normal.^[35]

Imaging Findings

• Usually, MRI and CT scans demonstrate normal structural finidings; in some cases, there may be cortical atrophy or demyelinating lesions.^[35]

EEG

• The most common EEG patern observed in Angelman syndrome are signals of high amplitude rhythmic 2–3 Hz activity (delta rythmicity) primarly over the frontal regions with superimposed interictal epileptiform discharges.^[39] Other patern found are rhythmic theta, and epileptiform spike-wave discharges.^[40]

Treatment

Medical Therapy

• Currently, there is no specific treatment for Angelman syndrome.^[41]
• Treatment is only supportive and is amied to:^[41][42]
  1. Mitigate gross and fine motor delays.^{[41][42][7][15]}
  2. Improve communication with non-verbal methods (eg. use of communication devices, implement a sign language, exchange of image cards).^{[41][42][7][15]}
  3. Intervention for autism spectrum disorder, when present.^{[41][42][7][15]}

• Feeding in newborns may requiere special nipples due to poor sucking.^[15][43]
• Antiepileptics are used for seizures, but there hasn't been a consensus on wich medication is the most appropiate.^[15][44][43]
• Stimulants (methylphenidate) have been used to control hyperactivity behaviours.^[15][41]
• Physiotherapy may improve range of movements and prevents joint stiffness.
• Occupational therapy helps to ameliorate fine motor and oral-motor control.^[15][43]
• Use of low-potency sedatives may help with disruptive nighttime wakefulness.^[15][45][41]
• Orthopedic postures may be corrected with bracing.^[15][43]
• Dietary recomendations should be made in patients with constipation and/or obesity.^[46][41]

Surgery

• Sometimes fundoplication may be requiered for reflux symptoms.^[15]
• Surgery may be needed to correct certain orthopedic problems (eg. severe scoliosis).^[15][43]
• Surgery for tongue protrusion has not found to be effective.^[15]

Prevention

• There are no primary preventive measures available for Angelman syndrome.

Living with Angelman syndrome

Although a diagnosis of Angelman syndrome is life-changing, it does not need to be life-destroying. Individuals with Angelman Syndrome are generally happy and contented individuals, who like human contact and play. Angelman syndrome individuals exhibit a profound desire for personal interaction with others. Communication can be difficult at first, but as an AS child develops, there is a definite character and ability to make themselves understood. It is widely accepted that their understanding of communication directed to them is much larger than their ability to return conversation.^[30]

See also

• Epigenetics

External links

• Template:Dmoz
• Angelman Syndrome at NIH/UW GeneTests
• Angelman Syndrome Foundation USA

References

Template:Chromosomal abnormalities

ca:Síndrome d'Angelman de:Angelman-Syndrom zh-classical:天使人症候群 he:תסמונת אנגלמן hu:Angelman-szindróma nl:Syndroom van Angelman sr:Ангелманов синдром fi:Angelmanin oireyhtymä sv:Angelmans syndrom

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