Dentatorubral–pallidoluysian atrophy
Congenital neurodegenerative disorder
| Dentatorubral–pallidoluysian atrophy | |
|---|---|
| |
| Synonyms | Haw River syndrome, Naito–Oyanagi disease |
| Pronounce | N/A |
| Field | Neurology, Genetics |
| Symptoms | Ataxia, choreoathetosis, myoclonus, seizures, dementia |
| Complications | Progressive neurodegeneration, epilepsy, loss of mobility |
| Onset | Childhood or adulthood (varies by CAG repeat length) |
| Duration | Lifelong |
| Types | Juvenile-onset, early adult-onset, late adult-onset |
| Causes | Mutation in the ATN1 gene |
| Risks | Family history of DRPLA |
| Diagnosis | Genetic testing, neuroimaging, clinical evaluation |
| Differential diagnosis | Huntington's disease, spinocerebellar ataxia, Lafora disease, sialidosis |
| Prevention | None |
| Treatment | Symptomatic management |
| Medication | Anticonvulsants, psychotropic medications |
| Prognosis | Progressive and variable |
| Frequency | Rare, more common in Japan |
| Deaths | Progressive neurodegeneration may lead to early death |
Dentatorubral–pallidoluysian atrophy (DRPLA) is a rare neurodegenerative disorder inherited in an autosomal dominant pattern. It is caused by a CAG repeat expansion in the ATN1 gene, which encodes the protein atrophin-1. The condition leads to progressive spinocerebellar degeneration and affects various parts of the central nervous system, including the dentate nucleus, red nucleus, globus pallidus, and subthalamic nucleus.
DRPLA is also known as Haw River syndrome or Naito–Oyanagi disease. It is most commonly found in individuals of Japanese descent but has been reported in other populations.
Clinical presentation[edit]
DRPLA has variable onset, categorized into three types:
- Juvenile-onset (before age 20): Presents with myoclonus, epilepsy, ataxia, and cognitive decline resembling progressive myoclonus epilepsy.
- Early adult-onset (age 20–40): Characterized by ataxia, seizures, and dementia.
- Late adult-onset (after age 40): Symptoms include choreoathetosis, ataxia, and cognitive impairment.
Additional features may include dystonia, sleep apnea, autism spectrum disorders, and corneal degeneration.
Genetics[edit]
The disorder is caused by a pathogenic expansion of the CAG trinucleotide repeat in the ATN1 gene on chromosome 12. Normal individuals have fewer than 35 repeats; those with DRPLA typically have more than 49. The expansion leads to an abnormally long polyglutamine tract in the atrophin-1 protein.
DRPLA shows genetic anticipation, where symptoms appear earlier and more severely in subsequent generations, particularly with paternal transmission.
Pathophysiology[edit]
The mutant atrophin-1 protein accumulates in neuronal nuclei and forms neuronal intranuclear inclusions (NIIs), which are associated with neurotoxicity. The inclusions are found throughout the brain, especially in the basal ganglia, cerebellum, and brainstem. The disease is marked by progressive brain atrophy and loss of neuronal function.
Diagnosis[edit]
Diagnosis is based on:
- Family history and clinical symptoms
- Genetic testing to confirm CAG repeat expansion in ATN1
- MRI to detect cerebral atrophy
- EEG to assess seizure activity
- Neuropsychological testing for cognitive decline
Differential diagnosis[edit]
Conditions that may mimic DRPLA include:
- Huntington's disease
- Spinocerebellar ataxias
- Lafora disease
- Neuronal ceroid lipofuscinosis
- Sialidosis
- Unverricht–Lundborg disease
Management[edit]
There is no cure for DRPLA. Management includes:
- Anticonvulsants for seizure control
- Psychotropic drugs for mood or psychotic symptoms
- Physical therapy and occupational therapy
- Supportive care for mobility and activities of daily living
Prognosis[edit]
DRPLA is progressive and leads to increasing neurological impairment. The rate of progression varies by age of onset and size of the CAG repeat expansion. Juvenile-onset cases generally have a more rapid and severe course.
Epidemiology[edit]
DRPLA is rare worldwide but more prevalent in Japan, with an estimated frequency of 2–7 per million people. The disorder is much less common in Western populations.
Related topics[edit]
- Trinucleotide repeat disorder
- Huntington's disease
- Spinocerebellar ataxia
- Neurodegeneration
- Ataxia
- Epilepsy
| Seizures and epilepsy | ||||||||||
|---|---|---|---|---|---|---|---|---|---|---|
|
| Non-Mendelian inheritance: anticipation | ||||||
|---|---|---|---|---|---|---|
|
Ad. Transform your health with W8MD Weight Loss, Sleep & MedSpa
Tired of being overweight?
Special offer:
Budget GLP-1 weight loss medications
- Semaglutide starting from $29.99/week and up with insurance for visit of $59.99 and up per week self pay.
- Tirzepatide starting from $45.00/week and up (dose dependent) or $69.99/week and up self pay
✔ Same-week appointments, evenings & weekends
Learn more:
- GLP-1 weight loss clinic NYC
- W8MD's NYC medical weight loss
- W8MD Philadelphia GLP-1 shots
- Philadelphia GLP-1 injections
- Affordable GLP-1 shots NYC
|
WikiMD Medical Encyclopedia |
Medical Disclaimer: WikiMD is for informational purposes only and is not a substitute for professional medical advice. Content may be inaccurate or outdated and should not be used for diagnosis or treatment. Always consult your healthcare provider for medical decisions. Verify information with trusted sources such as CDC.gov and NIH.gov. By using this site, you agree that WikiMD is not liable for any outcomes related to its content. See full disclaimer.
Credits:Most images are courtesy of Wikimedia commons, and templates, categories Wikipedia, licensed under CC BY SA or similar.
Translate this page: - East Asian
中文,
日本,
한국어,
South Asian
हिन्दी,
தமிழ்,
తెలుగు,
Urdu,
ಕನ್ನಡ,
Southeast Asian
Indonesian,
Vietnamese,
Thai,
မြန်မာဘာသာ,
বাংলা
European
español,
Deutsch,
français,
Greek,
português do Brasil,
polski,
română,
русский,
Nederlands,
norsk,
svenska,
suomi,
Italian
Middle Eastern & African
عربى,
Turkish,
Persian,
Hebrew,
Afrikaans,
isiZulu,
Kiswahili,
Other
Bulgarian,
Hungarian,
Czech,
Swedish,
മലയാളം,
मराठी,
ਪੰਜਾਬੀ,
ગુજરાતી,
Portuguese,
Ukrainian
