Huntington's Disease-Like 2 (HDL2)

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Huntington's Disease-Like 2 (HDL2)

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Huntington's Disease-Like 2 (HDL2)

Overview

Huntington's disease-like 2 (HDL2) is a rare autosomal dominant neurodegenerative disorder that phenotypically resembles Huntington's disease but is caused by a different genetic mutation. It was first described in 2004 in a large family from South Africa and is now recognized as an important cause of Huntington's disease-like syndrome worldwide[@walker2007]. HDL2 is caused by a CGG repeat expansion in the JPH3 (junctophilin-3) gene on chromosome 16q24.3[@margolis2004].

Pathway / Mechanism Diagram

graph TD A["HTT Gene: CAG Repeat Expansion"] --> B["Mutant Huntingtin (mHTT)"] B --> C["Polyglutamine Aggregation"] C --> D["Nuclear Inclusions"] B --> E["Transcriptional Dysregulation"] E --> F["BDNF Downregulation"] F --> G["Striatal Neuron Vulnerability"] B --> H["Mitochondrial Dysfunction"] H --> I["Energy Deficit"] B --> J["Impaired Autophagy"] J --> K["Toxic Protein Accumulation"] G --> L["Medium Spiny Neuron Death"] I --> L K --> L L --> M["Chorea and Motor Symptoms"] L --> N["Cognitive Decline"] L --> O["Psychiatric Symptoms"] style A fill:#ef5350,color:#e0e0e0 style L fill:#ef5350,color:#e0e0e0 style B fill:#5d4400,color:#e0e0e0

Genetics and Pathophysiology

...

Huntington's Disease-Like 2 (HDL2)

Overview

Huntington's disease-like 2 (HDL2) is a rare autosomal dominant neurodegenerative disorder that phenotypically resembles Huntington's disease but is caused by a different genetic mutation. It was first described in 2004 in a large family from South Africa and is now recognized as an important cause of Huntington's disease-like syndrome worldwide[@walker2007]. HDL2 is caused by a CGG repeat expansion in the JPH3 (junctophilin-3) gene on chromosome 16q24.3[@margolis2004].

Pathway / Mechanism Diagram

Mermaid diagram (expand to render)

Genetics and Pathophysiology

Genetic Basis

Inheritance: Autosomal dominant
Gene: JPH3 (junctophilin-3)
Mutation Type: CGG trinucleotide repeat expansion in the 5' UTR
Chromosomal Location: 16q24.3
Normal Repeat: 6-27 CGG repeats
Pathogenic Repeat: 41-58+ CGG repeats

Pathophysiology

The exact mechanism by which the JPH3 mutation leads to neurodegeneration remains incompletely understood. Several hypotheses have been proposed:

RNA-mediated toxicity: Expanded CGG repeats may form toxic RNA structures that sequester essential RNA-binding proteins
Repeat-associated non-AUG (RAN) translation: Production of toxic polyglycine-containing proteins
Loss of JPH3 function: Junctophilin-3 is involved in calcium homeostasis at the endoplasmic reticulum-mitochondria contact sites

JPH3 is expressed in [neurons](/entities/neurons) throughout the brain, particularly in the striatum and [cortex](/brain-regions/cortex), which are the primary regions affected in HDL2[@storey2015].

Clinical Presentation

HDL2 presents with clinical features almost identical to Huntington's disease:

Core Symptoms

Chorea: Involuntary, dance-like movements typically starting in the face and progressing to limbs

Cognitive decline: Executive dysfunction, memory impairment, and eventual dementia

Psychiatric disturbances: Depression, anxiety, irritability, and sometimes psychosis

Motor Features

Dysarthria (slurred speech)
Dysphagia (difficulty swallowing)
Gait disturbance and falls
Dystonia in later stages
Parkinsonism in some patients

Psychiatric Features

Depression (most common)
Anxiety disorders
Apathy
Impulse control problems
Less commonly, hallucinations and delusions

Disease Course

Age of onset: Typically 30-50 years, but can range from early 20s to late 60s
Disease duration: 10-20 years from symptom onset to death
Progression: Gradual decline in motor and cognitive function

A similar phenomenon to Huntington's disease is observed where larger repeat expansions are associated with earlier onset[@krause2007].

Diagnosis

Diagnostic Criteria

Adult-onset progressive chorea

Cognitive/behavioral decline

Family history consistent with autosomal dominant inheritance

Negative Huntington's disease testing (normal [HTT](/proteins/huntingtin) CAG repeat)

Positive JPH3 CGG repeat expansion

Genetic Testing

Molecular testing: PCR and fragment analysis to detect CGG repeat expansion in JPH3
Southern blotting: To confirm large expansions (>100 repeats)

Neuroimaging

MRI: Caudate nucleus and putamen atrophy, cortical atrophy in advanced cases
CT: May show striatal atrophy in moderate to advanced disease

Differential Diagnosis

Huntington's disease (HTT CAG expansion)
HDL1 (PRNP octapeptide insertions)
Spinocerebellar ataxias
Neuroacanthocytosis syndromes
Benign hereditary chorea
Drug-induced movement disorders

Treatment

Currently, there is no cure or disease-modifying therapy for HDL2. Treatment is supportive and symptomatic.

Chorea Management

Tetrabenazine: First-line for chorea control
Deutetrabenazine: Alternative with potentially better tolerability
Antipsychotics: Haloperidol, olanzapine, or risperidone

Psychiatric Symptoms

Depression: SSRIs (sertraline, citalopram)
Anxiety: Benzodiazepines or SSRIs
Psychosis: Atypical antipsychotics

Cognitive Symptoms

No effective pharmacologic treatments
Supportive care and cognitive rehabilitation

Supportive Care

Physical therapy: Exercise and fall prevention
Occupational therapy: Adaptive equipment and home modifications
Speech therapy: For dysarthria and dysphagia
Nutritional support: Diet modification and feeding assistance

Epidemiology

Prevalence: Very rare; estimated at <1 per million
Geographic distribution: Described in families from South Africa, the United States, and other countries
Ethnicity: Initially described in families of African descent, but now reported in multiple ethnic groups

Research Directions

Current Investigations

Pathogenesis studies: Understanding RNA toxicity and RAN translation

Biomarker development: Identifying fluid and imaging biomarkers

Therapeutic development:

Antisense oligonucleotides (ASOs) targeting JPH3
Small molecules to reduce toxic RAN translation
Gene therapy approaches

Animal Models

Mouse models with expanded CGG repeats in JPH3 are being developed
These models will be crucial for testing therapeutic interventions

References

[Walker RH, et al, Huntington disease-like 2 (2007)](https://pubmed.ncbi.nlm.nih.gov/17984064/)

[Margolis RL, et al, Huntington disease-like 2 (HDL2) (2004)](https://pubmed.ncbi.nlm.nih.gov/15479810/)

[Storey E, Bahlo M, Huntington disease-like 2: a clinicopathological case (2015)](https://pubmed.ncbi.nlm.nih.gov/25853748/)

[Krause A, et al, HDL2 in a South African population (2007)](https://pubmed.ncbi.nlm.nih.gov/17264702/)

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📊 Evidence Profile Foundational

Evidence Balance

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Certainty

95%

Debates

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Incoming

19

Outgoing

22

0 supporting 0 contradicting 0 neutral

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Huntington's Disease-Like 2 (HDL2)

Huntington's Disease-Like 2 (HDL2)

Overview

Pathway / Mechanism Diagram

Genetics and Pathophysiology

Huntington's Disease-Like 2 (HDL2)

Overview

Pathway / Mechanism Diagram

Genetics and Pathophysiology

Genetic Basis

Pathophysiology

Clinical Presentation

Core Symptoms

Motor Features

Psychiatric Features

Disease Course

Diagnosis

Diagnostic Criteria

Genetic Testing

Neuroimaging

Differential Diagnosis

Treatment

Chorea Management

Psychiatric Symptoms

Cognitive Symptoms

Supportive Care

Epidemiology

Research Directions

Current Investigations

Animal Models

See Also

References

💬 Discussion