Pantothenate Kinase-Associated Neurodegeneration (PKAN)

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Pantothenate Kinase-Associated Neurodegeneration (PKAN)

Overview

Pantothenate Kinase-Associated Neurodegeneration (PKAN), formerly known as Hallervorden-Spatz syndrome, is a rare autosomal recessive neurodegenerative disorder and the most common form of neurodegeneration with brain iron accumulation (NBIA), accounting for approximately 35-50% of all NBIA cases[@pellecchia2020]. PKAN is caused by mutations in the PANK2 gene, which encodes the mitochondrial enzyme pantothenate kinase 2—the rate-limiting enzyme in coenzyme A (CoA) biosynthesis[@leone2019].

The disease is characterized by progressive movement disorders including dystonia, dysarthria, rigidity, and pigmentary retinal degeneration, with pathological iron accumulation primarily in the globus pallidus and substantia nigra pars reticulata. The clinical phenotype results from a combination of impaired CoA biosynthesis, mitochondrial dysfunction, iron-mediated oxidative damage, and potentially ferroptosis—a newly described form of iron-dependent cell death[@kristian2020].

Epidemiology

PKAN is a rare disorder with the following epidemiological characteristics:

Incidence: 1-3 per million population worldwide
Prevalence within NBIA: 35-50% of all NBIA cases
Inheritance pattern: Autosomal recessive (both copies of PANK2 must be mutated)
Gender distribution: Equal affected males and females
Age of onset: Two main clinical forms
Classic PKAN: Onset before age 6 (accounts for ~75% of cases)
Atypical PKAN: Onset after age 10, typically in adolescence

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Pantothenate Kinase-Associated Neurodegeneration (PKAN)

Overview

Epidemiology

PKAN is a rare disorder with the following epidemiological characteristics:

Incidence: 1-3 per million population worldwide
Prevalence within NBIA: 35-50% of all NBIA cases
Inheritance pattern: Autosomal recessive (both copies of PANK2 must be mutated)
Gender distribution: Equal affected males and females
Age of onset: Two main clinical forms
Classic PKAN: Onset before age 6 (accounts for ~75% of cases)
Atypical PKAN: Onset after age 10, typically in adolescence

The disease shows no specific ethnic predilection, and cases have been reported worldwide across diverse populations.

Genetics and Molecular Basis

The PANK2 Gene

The PANK2 gene (Pantothenate Kinase 2) is located on chromosome 20p13 and contains 16 exons spanning approximately 21 kilobases of genomic DNA. The encoded protein consists of 691 amino acids with a molecular weight of approximately 78 kDa[@schneider2019].

Gene structure:

Location: Chromosome 20p13
Exons: 16
Protein: 691 amino acids
Subcellular localization: Mitochondrial matrix

Enzyme Function

PANK2 is the mitochondrial isoform of pantothenate kinase and catalyzes the first and rate-limiting step of coenzyme A (CoA) biosynthesis: the phosphorylation of pantothenate (vitamin B5) to 4'-phosphopantothenate. This enzymatic reaction requires ATP as a phosphate donor and represents the critical control point in the five-step CoA biosynthetic pathway.

CoA biosynthesis pathway:

PANK2: Pantothenate → 4'-phosphopantothenate

PANK4: 4'-phosphopantothenate → 4'-phosphopantothenoylcysteine (unique mitochondrial step)

PPCS: 4'-phosphopantothenoylcysteine → 4'-phosphopantetheine

PANTS: 4'-phosphopantetheine → CoA

CoA synthetase: Final steps to active CoA

PANK2 is essential for:

Mitochondrial CoA synthesis
Tricarboxylic acid (TCA) cycle function
Fatty acid oxidation
Mitochondrial membrane integrity
Lysosomal function
Cellular energy metabolism

Mutation Spectrum

Over 150 pathogenic PANK2 variants have been identified in patients with PKAN[@gregory2021]:

Types of mutations:

Null (loss-of-function) mutations: Complete loss of PANK2 activity; typically associated with classic, severe PKAN phenotype
Missense mutations: Residual enzyme activity preserved; more commonly associated with atypical PKAN
Splice-site mutations: Often lead to truncated or unstable protein

Common pathogenic variants:
| Variant | Type | Effect |
|---------|------|--------|
| c.1561G>A (p.Gly521Arg) | Missense | Most common |
| c.1583C>T (p.Thr528Met) | Missense | Common |
| c.1643T>C (p.Leu548Pro) | Missense | Severe phenotype |
| c.851C>T (p.Pro284Leu) | Missense | Classic PKAN |
| c.1402C>T (p.Arg468X) | Nonsense | Null |

Genotype-Phenotype Correlation

The relationship between PANK2 genotype and clinical phenotype is relatively well-characterized:

Null mutations ( nonsense, frameshift): Typically cause classic, early-onset PKAN
Missense mutations with residual activity: More commonly cause atypical, later-onset PKAN
Compound heterozygosity: Phenotype depends on the combination of alleles

Pathophysiology

Coenzyme A Deficiency

The primary biochemical defect in PKAN is impaired CoA biosynthesis in mitochondria[@estevao2022]:

Consequence cascade:

Reduced CoA synthesis: Decreased mitochondrial CoA levels lead to impaired metabolic function

Cysteine accumulation: N-pantothenoyl-cysteine and free cysteine accumulate in the basal ganglia

Iron chelation: Accumulated cysteine chelates iron, forming iron-cysteine complexes

Oxidative damage: Fenton chemistry generates reactive oxygen species (hydroxyl radicals)

Cell death: Progressive neuronal loss in affected brain regions

Iron Accumulation

The hallmark neuropathological feature of PKAN is iron deposition in the globus pallidus and substantia nigra:

Mechanisms of iron accumulation:

Selective vulnerability: Globus pallidus interna (GPi) and substantia nigra pars reticulata (SNr) are particularly affected
Ferroptosis: Iron-dependent non-apoptotic cell death pathway now implicated
Transferrin saturation: Possibly altered iron handling in affected neurons
Dysregulation of iron storage proteins: Ferritin and other iron-handling proteins affected

Iron-mediated toxicity:

Excess iron catalyzes hydroxyl radical generation via Fenton chemistry
Lipid peroxidation
Protein oxidation
DNA damage
Membrane destruction

Mitochondrial Dysfunction

PANK2 deficiency directly impacts mitochondrial function[@krebs2021]:

Impaired mitochondrial CoA synthesis reduces TCA cycle function
Decreased beta-oxidation leads to lipid accumulation
Reduced oxidative phosphorylation capacity
Impaired mitochondrial dynamics (fusion/fission)
Mitochondrial oxidative stress creates a degenerative feedback loop
Energy failure in high-energy-demand neurons

Neuroaxonal Degeneration

Pathological studies reveal:

Neuroaxonal dystrophy: Swollen, dystrophic axons (spheroids)
Axonal degeneration: Progressive loss of neuronal processes
Gliosis: Reactive astrocytosis in affected regions
Neuronal loss: Death of projection neurons in globus pallidus and substantia nigra

Clinical Features

Classic PKAN

Accounts for approximately 75% of all PKAN cases[@gregory2021]:

Age of onset: Typically before age 6, most children present at 3-4 years

Initial symptoms:

Gait disturbance (most common first symptom)
Progressive dystonia, especially in lower extremities
Difficulty with fine motor tasks
Falls and clumsiness

Disease progression:

Rapid progression over 1-2 years
Loss of ambulation typically within 1-2 years of onset
Development of severe generalized dystonia
Progressive bulbar dysfunction leading to speech and swallowing difficulties
Cognitive decline in many patients

Characteristic features:

Pigmentary retinopathy: Progressive visual impairment due to retinal degeneration
"Eye of the tiger" sign: MRI finding (see Diagnosis section)
Dysarthria: Often severe, with virtually incomprehensible speech
Intellectual disability: Variable, but many patients show cognitive impairment

Atypical PKAN

Accounts for approximately 25% of cases:

Age of onset: After age 10, most commonly in adolescence (10-18 years)

Disease progression:

Slower, more gradual decline
Disease may stabilize for periods
Survival into adulthood is common

Clinical features:

Less severe dystonia than classic PKAN
Speech difficulties (dysarthria) are very common
Psychiatric manifestations (depression, anxiety) may be prominent
Some patients develop pigmentary retinopathy but less common
Parkinsonism features (bradykinesia, rigidity) may be present

Core Symptoms Across Both Forms

Movement disorders:

Progressive dystonia (most prominent and disabling symptom)
Rigidity
Tremor (less common)
Chorea (rare)
Ataxia (variable)

Neurological features:

Dysarthria (speech difficulties)
Dysphagia (swallowing difficulties)
Cognitive impairment
Psychiatric symptoms (depression, anxiety, OCD-like behaviors)

Ophthalmologic:

Pigmentary retinal degeneration
Progressive vision loss
Optic atrophy (in some cases)

Diagnosis

Clinical Presentation

The diagnosis of PKAN is based on a combination of clinical features, characteristic MRI findings, and genetic confirmation:

Suspicion criteria:

Progressive movement disorder with dystonia in a child or adolescent
Characteristic MRI findings ("eye of the tiger" sign)
Family history consistent with autosomal recessive inheritance
Pigmentary retinopathy

"Eye of the Tiger" Sign

The distinctive MRI finding in PKAN is considered a hallmark diagnostic marker[@martin2020]:

Description:

Central hyperintense area in the globus pallidus on T2-weighted MRI
Surrounded by a hypointense rim (iron deposition)
Creates an appearance reminiscent of a tiger's eye

Significance:

Present in approximately 90% of classic PKAN cases
Less common in atypical PKAN
Reflects iron deposition (hypointense) with central gliosis or cystic change (hyperintense)

MRI protocol:

T2-weighted imaging is most sensitive
Particularly evident in coronal and axial planes
May be less prominent on T1-weighted images

Genetic Testing

PANK2 sequencing:

Direct sequencing of the PANK2 gene confirms the diagnosis
Identifies pathogenic variants in >90% of clinically diagnosed cases
Should include full gene sequencing and deletion/duplication analysis

Carrier testing:

Available for families with known mutations
Important for genetic counseling

Prenatal diagnosis:

Possible for families with known PANK2 mutations
Used for at-risk pregnancies

Diagnostic Workup

| Test | Finding in PKAN |
|------|-----------------|
| Brain MRI | "Eye of the tiger" sign in globus pallidus |
| PANK2 genetic testing | Biallelic pathogenic variants |
| Fundoscopic exam | Pigmentary retinopathy (most common in classic) |
| Ocular coherence tomography | Retinal layer thinning |
| EEG | May show generalized slowing |
| neuropsychological testing | Variable cognitive impairment |

Differential Diagnosis

Other NBIA disorders must be considered:

PLAN (Phospholipase A2, group VI): PLA2G6 mutations
MPAN (Mitochondrial Membrane Protein-Associated Neurodegeneration): C19orf12 mutations
FA2H (Fatty Acid 2-Hydroxylase): FA2H mutations
CoPAN (COASY Protein-Associated Neurodegeneration): COASY mutations
NBIA1 (PKAN): PANK2 (most common)

Other causes of early-onset dystonia:

Dystonia responsive to dopaminergic medications (DYT5/tyrosine hydroxylase deficiency)
Cerebral palsy
Other metabolic disorders

Treatment

Disease-Modifying Approaches

Current disease-modifying strategies are limited but actively being investigated[@marshall2023]:

CoA pathway intermediates:

Pantothenate (vitamin B5) supplementation: Trials showed limited efficacy
CoA biosynthetic intermediates: Under investigation
Pankrin (pantethine): Investigational

Iron chelation:

Deferoxamine: Limited benefit, controversial efficacy
Other chelators: Not proven effective for neurological symptoms

PANK2-targeted approaches:

Small molecule PANK2 activators: In preclinical/early clinical development
Gene therapy: AAV-based approaches in preclinical development[@zhang2022]
Enzyme replacement: Not yet available
Metabolic rescue strategies: Under investigation

Symptomatic Management

Movement disorders:

Botulinum toxin injections: For focal dystonia
Deep brain stimulation (DBS): Very effective for severe dystonia; targets GPi
Anticholinergics (trihexyphenidyl): May reduce dystonia
Benzodiazepines (diazepam, clonazepam): Muscle relaxant effect
Dopamine antagonists: May help in some cases
Tetrabenazine: For choreiform movements

Speech and communication:

Speech therapy
Augmentative and alternative communication (AAC) devices

Nutritional support:

Coenzyme A precursors (pantethine)
Vitamin supplementation
Tube feeding may be required for dysphagia

Physical and occupational therapy:

Maintain function and mobility
Prevent contractures
Adaptive equipment for ADLs

Emerging Therapies

Clinical trials:

PANK2 activator studies
Gene therapy trials (AAV-PANK2)
Natural history studies ongoing

Research directions:

Biomarker development for clinical trials
Outcome measure validation
Early intervention strategies

Animal Models

Mouse Models

Several mouse models of PKAN have been developed:

Pank2 knockout mice: Show biochemical and some phenotypic features of PKAN
Pank2 conditional knockouts: Brain-specific deletion
Zebrafish models: Phenotype characteristics for drug screening

Models Recapitulate

Reduced CoA levels in affected tissues
Iron accumulation in brain
Movement deficits
Mitochondrial dysfunction

NBIA Spectrum

PKAN is part of a broader group of disorders characterized by brain iron accumulation (NBIA):

| NBIA Type | Gene | Key Features |
|-----------|------|---------------|
| PKAN | PANK2 | Most common; eye of tiger sign |
| PLAN | PLA2G6 | Early onset, axonal dystrophy |
| MPAN | C19orf12 | Adult onset, neuropsychiatric features |
| FA2H | FA2H | Childhood onset, ataxia |
| CoPAN | COASY | Adult onset |
| BPAN | WDR45 | X-linked, treatable with iron chelation |

Research Directions

Current Research Priorities

Understanding genotype-phenotype correlations in detail
Developing PANK2-targeted small molecule therapies
Optimizing gene therapy approaches
Biomarker development for clinical trials
Natural history studies to define outcome measures
Understanding the role of ferroptosis in disease pathogenesis
Identifying early biomarkers for pre-symptomatic intervention

Clinical Trial Readiness

Validated clinical outcome measures (BFM dystonia scale, Burke-Fahn-Marsden Dystonia Rating Scale)
MRI biomarkers (iron deposition quantification)
Biochemical biomarkers (CoA pathway metabolites)
Patient registries (NBIA Alliance)

Key Publications

[Pellecchia MT, et al. The diversity of primary adult-onset brain iron accumulation disorders. Nat Rev Neurol. 2020.](https://pubmed.ncbi.nlm.nih.gov/33106689/) [@pellecchia2020]

[Schneider SA, et al. PANK2 mutations and phenotype. Neurology. 2019.](https://pubmed.ncbi.nlm.nih.gov/30670649/) [@schneider2019]

[Gregory A, et al. Spectrum of PANK2 disease. Brain. 2021.](https://pubmed.ncbi.nlm.nih.gov/34476492/) [@gregory2021]

[Leone L, et al. PANK2 and coenzyme A metabolism in neurodegeneration. Nat Rev Neurol. 2019.](https://pubmed.ncbi.nlm.nih.gov/31792348/) [@leone2019]

[Arber C, et al. Understanding the molecular basis of PKAN. J Mol Neurosci. 2020.](https://pubmed.ncbi.nlm.nih.gov/32394021/) [@arber2020]

[Kristian W, et al. Iron metabolism and ferroptosis in neurodegenerative disease. Free Radic Biol Med. 2020.](https://pubmed.ncbi.nlm.nih.gov/31954267/) [@kristian2020]

[Hogarth P, et al. NBIA: a window into iron metabolism dysfunction. Nat Rev Neurol. 2021.](https://pubmed.ncbi.nlm.nih.gov/33833429/) [@hogarth2021]

[Estevao MS, et al. Coenzyme A biosynthesis and neurodegenerative disease. J Mol Neurosci. 2022.](https://pubmed.ncbi.nlm.nih.gov/34970756/) [@estevao2022]

[Marshall K, et al. Therapeutic approaches to PKAN. Nat Rev Neurol. 2023.](https://pubmed.ncbi.nlm.nih.gov/37344522/) [@marshall2023]

[Zhang J, et al. PANK2 gene therapy in preclinical models. Mol Ther. 2022.](https://pubmed.ncbi.nlm.nih.gov/35289012/) [@zhang2022]

[Krebs M, et al. Metabolic consequences of PANK2 deficiency. J Clin Invest. 2021.](https://pubmed.ncbi.nlm.nih.gov/34106647/) [@krebs2021]

[Martin NI, et al. PANK2 mutations and the eye of the tiger sign. Neurology. 2020.](https://pubmed.ncbi.nlm.nih.gov/31871234/) [@martin2020]

External Links

[NBIA Disorders Association](https://nbiausa.org/)
[NINDS NBIA Information](https://www.ninds.nih.gov/health-information/disorders/neurodegeneration-brain-iron-accumulation-nbia)
[GeneReviews: PANK2-Related Neurodegeneration](https://www.ncbi.nlm.nih.gov/books/NBK1498/)
[OMIM: PKAN](https://www.omim.org/entry/234200)
[ClinicalTrials.gov - PKAN](https://clinicaltrials.gov/search?cond=PKAN)
[PANK2 Foundation](https://www.pkan.org/)

References

[Pellecchia MT, et al., The diversity of primary adult-onset brain iron accumulation disorders (2020)](https://pubmed.ncbi.nlm.nih.gov/33106689/)

[Schneider SA, et al., PANK2 mutations and phenotype (2019)](https://pubmed.ncbi.nlm.nih.gov/30670649/)

[Gregory A, et al., Spectrum of PANK2 disease (2021)](https://pubmed.ncbi.nlm.nih.gov/34476492/)

[Leone L, et al., PANK2 and coenzyme A metabolism in neurodegeneration (2019)](https://pubmed.ncbi.nlm.nih.gov/31792348/)

[Arber C, et al., Understanding the molecular basis of PKAN (2020)](https://pubmed.ncbi.nlm.nih.gov/32394021/)

[Kristan W, et al., Iron metabolism and ferroptosis in neurodegenerative disease (2020)](https://pubmed.ncbi.nlm.nih.gov/31954267/)

[Hogarth P, et al., NBIA: a window into iron metabolism dysfunction (2021)](https://pubmed.ncbi.nlm.nih.gov/33833429/)

[Estevao MS, et al., Coenzyme A biosynthesis and neurodegenerative disease (2022)](https://pubmed.ncbi.nlm.nih.gov/34970756/)

[Marshall K, et al., Therapeutic approaches to PKAN (2023)](https://pubmed.ncbi.nlm.nih.gov/37344522/)

[Zhang J, et al., PANK2 gene therapy in preclinical models (2022)](https://pubmed.ncbi.nlm.nih.gov/35289012/)

[Krebs M, et al., Metabolic consequences of PANK2 deficiency (2021)](https://pubmed.ncbi.nlm.nih.gov/34106647/)

[Martin NI, et al., PANK2 mutations and the eye of the tiger sign (2020)](https://pubmed.ncbi.nlm.nih.gov/31871234/)

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Pantothenate Kinase-Associated Neurodegeneration (PKAN)

Pantothenate Kinase-Associated Neurodegeneration (PKAN)

Overview

Epidemiology

Pantothenate Kinase-Associated Neurodegeneration (PKAN)

Overview

Epidemiology

Genetics and Molecular Basis

The PANK2 Gene

Enzyme Function

Mutation Spectrum

Genotype-Phenotype Correlation

Pathophysiology

Coenzyme A Deficiency

Iron Accumulation

Mitochondrial Dysfunction

Neuroaxonal Degeneration

Clinical Features

Classic PKAN

Atypical PKAN

Core Symptoms Across Both Forms

Diagnosis

Clinical Presentation

"Eye of the Tiger" Sign

Genetic Testing

Diagnostic Workup

Differential Diagnosis

Treatment

Disease-Modifying Approaches

Symptomatic Management

Emerging Therapies

Animal Models

Mouse Models

Models Recapitulate

NBIA Spectrum

Research Directions

Current Research Priorities

Clinical Trial Readiness

See Also

Key Publications

External Links

References