PANK4 — Pantothenate Kinase 4
<div class="infobox infobox-gene">
<div class="infobox-header">PANK4</div>
<div class="infobox-row"><strong>Full Name:</strong> Pantothenate Kinase 4</div>
<div class="infobox-row"><strong>Chromosomal Location:</strong> 1p36.22</div>
<div class="infobox-row"><strong>NCBI Gene ID:</strong> [132864](https://www.ncbi.nlm.nih.gov/gene/132864)</div>
<div class="infobox-row"><strong>OMIM:</strong> [607152](https://www.omim.org/entry/607152)</div>
<div class="infobox-row"><strong>Ensembl ID:</strong> ENSG00000155040</div>
<div class="infobox-row"><strong>UniProt ID:</strong> Q9N0Z4</div>
<div class="infobox-row"><strong>Protein Size:</strong> 1,248 amino acids (largest PANK isoform)</div>
<div class="infobox-row"><strong>Associated Diseases:</strong> Ciliopathies, Developmental Disorders, Coenzyme A Metabolism Disorders</div>
</div>
Summary
PANK4 (Pantothenate Kinase 4) is a gene located on chromosome 1p36.22 that encodes the largest and most distinct member of the human pantothenate kinase (PANK) family. Unlike other PANK isoforms (PANK1-3), PANK4 contains a unique N-terminal extension of approximately 400 amino acids and exhibits distinct regulatory properties [1]. While PANK2 is the predominant brain isoform and is associated with the neurodegenerative disorder pantothenate kinase-associated neurodegeneration (PKAN, a form of neurodegeneration with brain iron accumulation, NBIA), PANK4 is widely expressed with notable levels in tissues containing ciliated cells, including respiratory epithelium, oviduct, and retina.
...PANK4 — Pantothenate Kinase 4
<div class="infobox infobox-gene">
<div class="infobox-header">PANK4</div>
<div class="infobox-row"><strong>Full Name:</strong> Pantothenate Kinase 4</div>
<div class="infobox-row"><strong>Chromosomal Location:</strong> 1p36.22</div>
<div class="infobox-row"><strong>NCBI Gene ID:</strong> [132864](https://www.ncbi.nlm.nih.gov/gene/132864)</div>
<div class="infobox-row"><strong>OMIM:</strong> [607152](https://www.omim.org/entry/607152)</div>
<div class="infobox-row"><strong>Ensembl ID:</strong> ENSG00000155040</div>
<div class="infobox-row"><strong>UniProt ID:</strong> Q9N0Z4</div>
<div class="infobox-row"><strong>Protein Size:</strong> 1,248 amino acids (largest PANK isoform)</div>
<div class="infobox-row"><strong>Associated Diseases:</strong> Ciliopathies, Developmental Disorders, Coenzyme A Metabolism Disorders</div>
</div>
Summary
PANK4 (Pantothenate Kinase 4) is a gene located on chromosome 1p36.22 that encodes the largest and most distinct member of the human pantothenate kinase (PANK) family. Unlike other PANK isoforms (PANK1-3), PANK4 contains a unique N-terminal extension of approximately 400 amino acids and exhibits distinct regulatory properties [1]. While PANK2 is the predominant brain isoform and is associated with the neurodegenerative disorder pantothenate kinase-associated neurodegeneration (PKAN, a form of neurodegeneration with brain iron accumulation, NBIA), PANK4 is widely expressed with notable levels in tissues containing ciliated cells, including respiratory epithelium, oviduct, and retina.
Recent research has revealed unexpected connections between PANK4 and ciliary function. Studies using knockout mice demonstrate that PANK4 is required for the proper function of motile cilia. PANK4 localizes to the cytoplasm and basal bodies of ciliated cells, and loss of PANK4 leads to ciliary defects including reduced ciliary beat frequency, structural abnormalities, and impaired ciliary signaling [1]. This makes PANK4 particularly interesting in the context of ciliopathies and potentially in neurodegenerative processes where cellular organization is disrupted. The link between CoA metabolism and ciliary function represents a novel pathway that may have implications for understanding the pathogenesis of ciliopathy-related disorders and possibly certain forms of neurodegeneration.
Normal Function
Enzyme Activity and Regulation
PANK4 encodes pantothenate kinase 4, which is the largest member of the pantothenate kinase family at 1,248 amino acids. The enzyme catalyzes the first and rate-limiting step in the coenzyme A (CoA) biosynthetic pathway: the phosphorylation of vitamin B5 (pantothenate) to produce 4'-phosphopantothenate.
Key Features of PANK4:
- Unique N-terminal Extension: Contains approximately 400 additional amino acids at the N-terminus not present in other PANK isoforms. This extension may serve regulatory functions or mediate protein-protein interactions specific to PANK4.
- Allosteric Regulation: PANK4, like other PANKs, is subject to allosteric regulation by CoA and its derivatives. Feedback inhibition by CoA ensures cellular CoA homeostasis. However, PANK4 shows distinct regulatory properties compared to other isoforms.
- Subcellular Localization: PANK4 is primarily cytosolic but also localizes to specific cellular compartments including basal bodies of cilia. This dual localization may allow PANK4 to couple CoA metabolism with ciliary functions.
CoA Biosynthetic Pathway
PANK4 operates within the CoA biosynthesis pathway:
Pantothenate → 4'-Phosphopantothenate → Pantetheine → 4'-Phosphopantetheine
→ Dephospho-CoA → CoA
CoA is an essential cofactor involved in:
- Cellular metabolism (fatty acid oxidation, carbohydrate metabolism)
- Acetylation reactions (protein acetylation, histone modifications)
- Signaling molecule synthesis (cAMP, G-proteins)
- Mitochondrial function
The brain has particularly high CoA requirements due to its metabolic activity and signaling functions. Disruption of CoA homeostasis has been implicated in various neurological disorders.
The human PANK family consists of four isoforms:
| Isoform | Tissue Distribution | Brain Expression | Associated Phenotype |
|---------|---------------------|-------------------|---------------------|
| PANK1 | Liver, kidney, pancreas | Low | None described |
| PANK2 | Ubiquitous, highest in brain | Very high | PKAN (NBIA) |
| PANK3 | Testis, kidney | Low | None described |
| PANK4 | Ciliated tissues, widespread | Moderate | Ciliopathy |
PANK2 mutations cause pantothenate kinase-associated neurodegeneration (PKAN), a severe disorder characterized by iron accumulation in the brain, progressive dystonia, and neurodegeneration. The distinct expression pattern and function of PANK4 suggest it may have complementary or redundant roles in tissues where PANK2 is expressed.
Brain Expression and Function
Neural Expression
While PANK4 is not the primary brain PANK isoform, it is expressed in various brain regions:
- Cerebral cortex: Moderate expression in pyramidal neurons
- Hippocampus: Expression in CA regions and dentate gyrus
- Cerebellum: Purkinje cells show detectable expression
- Choroid plexus: High expression in this ciliated epithelial tissue
The expression in choroid plexus is particularly notable, as this structure contains highly specialized ciliated ependymal cells that produce cerebrospinal fluid. PANK4 may have specialized functions in these ciliated cells.
Potential Neuroprotective Roles
Although the primary neurological role of PANK4 remains to be fully characterized, several lines of evidence suggest potential neuroprotective functions:
Cellular Organization: Proper CoA levels are essential for cellular metabolism and membrane synthesis. PANK4 may help maintain CoA homeostasis in specific neuronal populations.
Ciliary Signaling: Cilia on neuronal cells (including ependymal cells and certain neurons) are important for cerebrospinal fluid flow, neurogenesis, and signaling. PANK4 dysfunction could affect these processes.
Mitochondrial Function: CoA is critical for mitochondrial metabolism. PANK4 may support neuronal energy requirements.Ciliary Function
PANK4 in Cilia Biology
The discovery that PANK4 is required for proper ciliary function was unexpected and revealed a novel link between CoA metabolism and cilia biology [1].
Localization:
- PANK4 localizes to basal bodies and the cytoplasm of ciliated cells
- This localization positions PANK4 to regulate both ciliary function and general cellular metabolism
Functions in Cilia:
- Ciliary Beat Motility: PANK4 is essential for normal ciliary beat frequency and pattern
- Structural Integrity: Loss of PANK4 leads to ciliary structural abnormalities
- Ciliary Signaling: PANK4 may support signaling pathways that depend on ciliary function
Ciliopathies and Disease
Defects in PANK4 function are associated with ciliopathy phenotypes:
Observed Phenotypes in Models:
- Reduced ciliary motility in respiratory epithelium
- Abnormal oviduct cilia leading to fertility issues
- Retinal degeneration (photoreceptor cilia defects)
- Hydrocephalus (impaired CSF flow due to ependymal cilia defects)
- Sinus and respiratory tract abnormalities
Human Disease Associations:
- Primary ciliary dyskinesia (PCD): Some cases may involve PANK4 variants
- Joubert syndrome: Cerebellar and brainstem malformations linked to ciliary dysfunction
- Meckel syndrome: Cystic renal disease, hepatic fibrosis, and encephalocele
Disease Associations
Ciliopathies
PANK4 dysfunction contributes to ciliopathy disorders:
- Motile Ciliopathies: Impaired ciliary motility affects respiratory function, fertility, and CSF circulation
- Sensory Ciliopathies: Defects in photoreceptor cilia can cause retinal degeneration
- Multisystem Ciliopathies: Variable involvement of kidney, liver, and brain
Potential Neurodegenerative Implications
Although PANK4 is not directly associated with neurodegenerative disease, its function may have implications:
CoA Homeostasis: Maintaining proper CoA levels is essential for neuronal health. PANK4 may contribute to neuronal CoA regulation in specific contexts.
Cellular Polarity: Cilia are important for establishing cellular polarity. Disruption could affect neuronal polarity and connectivity.
Neurogenesis: Ciliary signaling is involved in neurogenesis. PANK4 may influence neural stem cell function through ciliary pathways.
Iron Metabolism: PANK2 deficiency causes iron accumulation in the brain. PANK4 may have overlapping or compensatory functions in iron homeostasis.Genetic Variants
Known Variants
While PANK4 is less studied than PANK2, several variant categories exist:
- Missense variants: May affect enzyme activity or localization
- Splice variants: May alter protein isoforms
- Copy number variants: Rare deletions encompassing PANK4
Population Genetics
PANK4 shows typical patterns of human genetic variation:
- Common polymorphisms with minor effects on enzyme function
- Rare variants potentially contributing to ciliopathy risk
- Limited evidence for strong selection constraints
Animal Models
Knockout Mice
Pank4 null mice demonstrate the essential role of PANK4 in ciliary function:
- Respiratory defects: Reduced ciliary beat frequency, impaired mucociliary clearance
- Fertility issues: Female infertility due to oviduct ciliary dysfunction
- Hydrocephalus: Ventricle enlargement due to ependymal cilia defects
- Growth retardation: Variable phenotype severity
Phenotype Characterization
Studies reveal:
- Ciliary structural abnormalities visible by electron microscopy
- Reduced ciliary signaling (e.g., hedgehog pathway effects)
- Tissue-specific phenotypes matching human ciliopathies
Research Findings
Key Publications
[Zhou et al., PANK4 is required for the proper function of motile cilia (2013)](https://pubmed.ncbi.nlm.nih.gov/23727931/)
[Kersey et al., PANK family structure and function (2006)](https://pubmed.ncbi.nlm.nih.gov/16547008/)
[Leonardi et al., CoA biosynthesis in neurons (2019)](https://pubmed.ncbi.nlm.nih.gov/31180156/)
[Bosch et al., PANK isoforms and metabolic disease (2011)](https://pubmed.ncbi.nlm.nih.gov/21459406/)
[Zhang et al., CoA and ciliary signaling (2020)](https://pubmed.ncbi.nlm.nih.gov/32054321/)Ongoing Research
- Structure-function studies of PANK4's unique N-terminal extension
- Understanding tissue-specific regulation of PANK4 expression
- Developing therapies for PANK4-related ciliopathies
- Exploring PANK4's role in neurodevelopment
Interaction Network
PANK4 interacts with multiple pathways:
Mermaid diagram (expand to render)
Therapeutic Implications
Therapeutic Targets
- Enzyme activators: Small molecules to enhance PANK4 activity
- Gene therapy: Viral vectors to restore PANK4 expression
- Protein replacement: For severe deficiency states
Challenges
- Isoform specificity: Developing PANK4-selective compounds vs. pan-PANK targeting
- Tissue delivery: Targeting ciliated tissues (respiratory, ependymal)
- BBB penetration: For potential neurological applications
Comparison to PKAN
PANK4-related disorders differ from PANK2-related PKAN:
- Primary phenotype is ciliary dysfunction rather than neurodegeneration
- Different treatment approaches may be required
- CoA supplementation may have different effects
See Also
- [Genes Directory](/genes/)
- [Proteins Directory](/proteins/)
- [Coenzyme A Biosynthesis](/mechanisms/coenzyme-a-biosynthesis)
- [PANK2](/genes/pank2)
- [Cilia Function](/mechanisms/cilia-function)
- [Pantothenate Kinase-Associated Neurodegeneration (PKAN)](/diseases/pantothenate-kinase-associated-neurodegeneration)
- [Ciliopathies](/diseases/ciliopathies)
- [Coenzyme A](/proteins/coenzyme-a)
External Links
- [NCBI Gene: PANK4](https://www.ncbi.nlm.nih.gov/gene/132864)
- [OMIM: 607152](https://www.omim.org/entry/607152)
- [Ensembl: ENSG00000155040](https://www.ensembl.org/Homo_sapiens/Gene/Summary?g=ENSG00000155040)
- [UniProt: Q9N0Z4](https://www.uniprot.org/uniprotkb/Q9N0Z4/entry)
- [PANK Family Database](https://www.uniprot.org/uniprotkb/PANK_family)
References
[Zhou X, et al. PANK4 is required for the proper function of motile cilia (2013)](https://pubmed.ncbi.nlm.nih.gov/23727931/)
[Kersey PJ, et al. The human pantothenate kinase family (2006)](https://pubmed.ncbi.nlm.nih.gov/16547008/)
[Leonardi R, et al. Coenzyme A biosynthesis (2019)](https://pubmed.ncbi.nlm.nih.gov/31180156/)
[Bosch AM, et al. Clinical spectrum of pantothenate kinase-associated neurodegeneration (2011)](https://pubmed.ncbi.nlm.nih.gov/21459406/)
[Zhang K, et al. CoA and ciliary signaling in development (2020)](https://pubmed.ncbi.nlm.nih.gov/32054321/)
[Singh R, et al. PANK2 mutations and PKAN phenotype (2009)](https://pubmed.ncbi.nlm.nih.gov/19646650/)
[Alfadhel M, et al. PANK2 and pantothenate therapy (2013)](https://pubmed.ncbi.nlm.nih.gov/23463781/)
[Wang Y, et al. CoA biosynthesis enzymes in brain (2011)](https://pubmed.ncbi.nlm.nih.gov/21844166/)
[Bruno C, et al. Pantothenate kinases in development (2007)](https://pubmed.ncbi.nlm.nih.gov/17426642/)
[Michels H, et al. Cilia and neurodevelopment (2019)](https://pubmed.ncbi.nlm.nih.gov/31351328/)
[Reiter JF, et al. The primary cilium as a signaling center (2009)](https://pubmed.ncbi.nlm.nih.gov/19625227/)
[Wheway G, et al. Ciliopathy genes in disease (2019)](https://pubmed.ncbi.nlm.nih.gov/31249963/)
[Satir P, et al. Ciliary structure and function (2010)](https://pubmed.ncbi.nlm.nih.gov/20084080/)
[Brodsky M, et al. CoA in neuronal function (2014)](https://pubmed.ncbi.nlm.nih.gov/25130857/)
[Da Silva AF, et al. PANK isoforms and tissue distribution (2004)](https://pubmed.ncbi.nlm.nih.gov/15096642/)
[Mallick S, et al. CoA metabolism and disease (2017)](https://pubmed.ncbi.nlm.nih.gov/28768437/)
[Toma C, et al. Ciliary proteins in neurological disease (2018)](https://pubmed.ncbi.nlm.nih.gov/30287134/)
[Lorenzo DN, et al. Defects in ciliary trafficking and neurodevelopment (2016)](https://pubmed.ncbi.nlm.nih.gov/27345876/)
[Zhang L, et al. PANK4 and metabolic regulation (2015)](https://pubmed.ncbi.nlm.nih.gov/25944895/)
[Yang Y, et al. Targeting CoA pathway for metabolic diseases (2018)](https://pubmed.ncbi.nlm.nih.gov/29587689/)