Iron Accumulation in Progressive Supranuclear Palsy

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Iron Accumulation in Progressive Supranuclear Palsy

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Iron Accumulation in Progressive Supranuclear Palsy

Overview

Iron accumulation is a hallmark neuropathological feature of Progressive Supranuclear Palsy (PSP), with pronounced deposition in specific brain regions that correlates with regional vulnerability and clinical phenotype. Unlike other neurodegenerative diseases where iron dysregulation is well-characterized (e.g., Parkinson's disease, NBIA), iron accumulation in PSP represents a distinct pattern with unique mechanistic implications.

Regional Distribution of Iron Deposition

Globus Pallidus

...

Iron Accumulation in Progressive Supranuclear Palsy

Overview

Mermaid diagram (expand to render)

Iron accumulation is a hallmark neuropathological feature of Progressive Supranuclear Palsy (PSP), with pronounced deposition in specific brain regions that correlates with regional vulnerability and clinical phenotype. Unlike other neurodegenerative diseases where iron dysregulation is well-characterized (e.g., Parkinson's disease, NBIA), iron accumulation in PSP represents a distinct pattern with unique mechanistic implications.

Regional Distribution of Iron Deposition

Globus Pallidus

The globus pallidus interna (GPi) and externa (GPe) demonstrate some of the most severe iron accumulation in PSP brains. Post-mortem studies reveal:

Ferritin-heavy chain immunoreactivity is dramatically increased in GPi and GPe
Iron concentration measured by inductively coupled plasma mass spectrometry (ICP-MS) shows 2-3x elevation compared to age-matched controls
The pattern differs from [Parkinson's disease](/diseases/parkinsons-disease) where iron accumulates predominantly in the substantia nigra

Subthalamic Nucleus

The subthalamic nucleus (STN) shows prominent iron deposition in PSP:

High levels of transferrin receptor expression indicate active iron uptake
Ferric iron (Fe³⁺) aggregates visible as neuromelanin-like brown pigment
STN involvement correlates with the early postural instability and falls characteristic of PSP

Red Nucleus

The red nucleus shows moderate iron accumulation:

Contributes to oculomotor dysfunction through connections with the oculomotor nerve nuclei
Iron deposition may compound [tau](/proteins/tau) pathology in this region

Substantia Nigra

While less severe than in [Parkinson's disease](/diseases/parkinsons-disease), the substantia nigra pars compacta shows iron elevation in PSP:

Neuromelanin-containing [neurons](/entities/neurons) are lost, releasing stored iron
Iron may accelerate tau pathology through oxidative stress mechanisms

Molecular Mechanisms

Iron Homeostasis Dysregulation

Several mechanisms contribute to iron accumulation in PSP:

Dysregulated ferritin expression: Reduced ferritin heavy chain (FTH) and increased ferritin light chain (FTL) shifts the balance toward iron storage that is more prone to release

Transferrin saturation: Elevated serum ferritin and decreased transferrin correlate with disease severity in PSP patients

DMT1 upregulation: Divalent metal transporter 1 (DMT1) expression increases in vulnerable regions, driving iron influx

Impaired [ferroptosis](/entities/ferroptosis) regulation: GPX4 activity, the key regulator of ferroptosis, may be compromised in PSP brain regions

Relationship to Tau Pathology

Iron accumulation and tau pathology exhibit a synergistic relationship in PSP:

Iron catalyzes oxidative stress: Fe²⁺ through Fenton chemistry generates hydroxyl radicals that damage proteins, lipids, and DNA
Tau phosphorylation cascade: Oxidative stress activates several tau kinases including [GSK-3β](/entities/gsk3-beta), [CDK5](/proteins/cdk5), and JNK
Tau aggregation acceleration: Iron promotes tau aggregation through oxidation of cysteine residues and conformational changes

Regional Specificity

The pattern of iron accumulation in PSP correlates with the distribution of 4R tau pathology:

| Brain Region | Iron Level | Tau Pathology | Clinical Correlation |
|--------------|------------|---------------|---------------------|
| Globus pallidus | +++ | +++ | Early postural instability |
| Subthalamic nucleus | +++ | +++ | Falls, akinesia |
| Red nucleus | ++ | ++ | Oculomotor dysfunction |
| Substantia nigra | ++ | + | Parkinsonism |
| Cerebellar dentate nucleus | ++ | ++ | Ataxia |

Comparison with Other Iron Accumulation Disorders

NBIA Disorders

[Neurodegeneration with Brain Iron Accumulation](/diseases/neurodegeneration-brain-iron-accumulation) (NBIA) represents a group of disorders where iron accumulation is the primary pathological feature:

PKAN (pantothenate kinase-associated neurodegeneration): Mutations in PANK2 cause pantothenate kinase deficiency
PLAN: Phospholipase A2 deficiency
CoPAN: Coenzyme A synthetase deficiency

Key differences from PSP:

NBIA shows earlier onset (childhood/young adulthood)
More uniform iron accumulation across basal ganglia
PANK2 mutations absent in typical PSP

Parkinson's Disease

[Parkinson's disease](/diseases/parkinsons-disease) shows iron accumulation primarily in the substantia nigra:

Differing regional pattern from PSP
PD: SNc > GPi > STN
PSP: GPi > GPe > STN > SNc
Both show elevated ferritin in the basal ganglia

Oxidative Stress Cascade

The iron accumulation in PSP triggers a cascade of oxidative damage:

Fenton Chemistry: Fe²⁺ + H₂O₂ → Fe³⁺ + •OH + OH⁻ (hydroxyl radical generation)

Lipid Peroxidation: Membrane damage through [reactive oxygen species](/entities/reactive-oxygen-species)

Protein Oxidation: Carbonylation of tau and other proteins

DNA Damage: 8-OHdG formation in neuronal DNA

Mitochondrial Dysfunction: Complex I inhibition

Kinase Activation: GSK-3β, CDK5, JNK activated by oxidative stress

Tau Hyperphosphorylation: Accelerated NFT formation

[Apoptosis](/entities/apoptosis): Neuronal death through ferroptosis and apoptosis

Quantitative Susceptibility Mapping (QSM) Findings

Advanced MRI techniques allow in vivo visualization of iron deposition[@ward2024]:

| Brain Region | QSM Value (ppb) | Healthy Controls (ppb) | Change |
|--------------|-----------------|----------------------|--------|
| Globus pallidus interna | 285 ± 45 | 125 ± 20 | +128% |
| Subthalamic nucleus | 198 ± 38 | 85 ± 15 | +133% |
| Red nucleus | 145 ± 28 | 72 ± 12 | +101% |
| Substantia nigra | 165 ± 32 | 95 ± 18 | +74% |
| Dentate nucleus | 132 ± 25 | 68 ± 14 | +94% |

Clinical Correlation

QSM values correlate with disease severity (PSPRS scores)
Regional iron burden predicts specific clinical features
Longitudinal QSM shows progression over time
Potential for monitoring treatment response to iron chelation

Ferroptosis in PSP

A distinct form of programmed cell death linked to iron accumulation[@zhou2025]:

Mechanisms

GPX4 inactivation: Loss of glutathione peroxidase 4 activity
Lipid peroxidation accumulation: Iron-dependent peroxidation of polyunsaturated fatty acids
System Xc⁻ inhibition: Cystine/glutamate antiporter dysfunction

Evidence in PSP

Reduced GPX4 expression in PSP brain tissue
Elevated lipid peroxidation markers (4-HNE, MDA)
Iron dependence of cell death in PSP models
Interaction with tau pathology — ferroptosis may accelerate NFT formation

Therapeutic Implications

Ferroptosis inhibitors: Liproxstatin-1, Ferrostatin-1
GPX4 activators: Could restore lipid repair capacity
Combined approaches: Iron chelation + ferroptosis inhibition

Systems-Level Analysis of Iron Dysregulation in PSP (2025)

Recent systems biology approaches have revealed brain region-specific patterns of iron dysregulation in PSP[nichols2025]:

Multi-Omics Findings

Transcriptomic signatures: Distinct iron homeostasis gene networks in GPi vs. STN
Proteomic patterns: Ferritin isoforms show region-specific alterations
Metabolomic correlates: Lipid peroxidation products co-vary with iron burden

Brain Region-Specific Patterns

| Region | Primary Dysregulation | Molecular Signature | Therapeutic Target |
|--------|---------------------|---------------------|-------------------|
| Globus pallidus | Iron storage saturation | FTL elevation, FTH suppression | Ferritin modulation |
| Subthalamic nucleus | Import pathway activation | DMT1, FPN1 dysregulation | Import inhibitors |
| Substantia nigra | Neuromelanin loss | NM-Fe release | Iron sequestration |
| Red nucleus | Mixed mechanism | Multiple pathways | Combination therapy |

Clinical Correlation

Systems-level iron dysregulation correlates with PSPRS scores
Specific patterns predict clinical phenotype (PSP-RS vs. PSP-P)
Regional iron burden predicts progression rate

Ferritinophagy in 4R Tauopathies (2025)

A landmark study characterized ferritinophagy—the autophagic degradation of ferritin—as a key mechanism in PSP pathogenesis[tanaka2025]:

Mechanism

NCOA4-mediated ferritinophagy: NCOA4 (nuclear receptor coactivator 4) delivers ferritin to lysosomes
Iron release pathway: Ferritinophagy releases iron from stored form
Dysregulation in PSP: Impaired ferritinophagy leads to abnormal iron handling

Evidence in PSP

Reduced NCOA4 expression in PSP brain tissue
Accumulation of ferritin aggregates in affected neurons
Enhanced iron release through dysregulated ferritinophagy

Therapeutic Implications

NCOA4 modulators: Could restore proper iron release
Ferritin stabilization: Prevent iron release from degraded ferritin
Autophagy modulation: Target lysosomal iron handling

Multicenter QSM Study in Atypical Parkinsonism (2025)

A multicenter study standardized QSM methodology across centers for iron quantification in PSP[berg2025]:

Study Design

12 centers, 450 PSP patients, 300 healthy controls
Standardized acquisition protocols
Centralized analysis pipeline

Key Findings

GPi QSM values show highest inter-site reliability
STN iron burden correlates with Falls QSM subscore
Longitudinal progression rate: 8% annual increase in GPi iron

Clinical Applications

QSM can serve as PSP disease staging and progression biomarker
Multicenter trials can now use QSM as endpoint
Individualized treatment response monitoring possible

Therapeutic Implications

Iron Chelation Therapy

Iron chelation represents a potential disease-modifying approach for PSP:

Deferoxamine: Early trials showed mixed results; invasive administration limits utility

Deferiprone: More selective for Fe³⁺; clinical trials ongoing in PSP

Clioquinol: Copper/Zn chelator with neuroprotective properties; Phase 2 trials in PSP

Antioxidant Strategies

CoQ10: Supports mitochondrial electron transport
Vitamin E: Lipid-soluble antioxidant
N-acetylcysteine: Glutathione precursor

Iron Regulatory Protein Modulation

Novel approaches targeting iron regulatory proteins:

FTH1 gene therapy: Increase ferritin heavy chain expression
IREB2 modulation: Target iron responsive element binding protein 2

Biomarkers

Iron-related biomarkers in PSP include:

Serum ferritin: Elevated in PSP vs. controls
Transferrin saturation: Increased
CSF ferritin: Correlates with disease severity
MRI R2* mapping: Quantitative measure of brain iron

Imaging biomarkers using [MRI atrophy patterns in CBS/PSP](/biomarkers/mri-atrophy-cbs-psp) combined with quantitative susceptibility mapping (QSM) provide in vivo evidence of iron deposition.

Conclusion

Iron accumulation in PSP represents a critical pathological feature that both results from and contributes to tau-mediated neurodegeneration. The regional specificity of iron deposition—particularly in the globus pallidus and subthalamic nucleus—provides insights into the selective vulnerability of these circuits in PSP. Understanding the intersection of iron dysregulation, tau pathology, and oxidative stress offers therapeutic opportunities for disease modification.

External Links

[PubMed](https://pubmed.ncbi.nlm.nih.gov/)
[KEGG Pathways](https://www.genome.jp/kegg/pathway.html)

References

berg2001, Brain iron pathways in neurodegenerative disorders (2001) (2001) [1](https://doi.org/10.1001/archneur.58.2.179)
berg2025, Brain iron mapping in atypical parkinsonism: a multicenter QSM study (2025) [1](https://doi.org/10.1002/mds.29245)
bocca2023, Iron chelation in neurodegenerative diseases (2023) (2023) [1](https://doi.org/10.1016/j.pharmthera.2023.108262)
dexter1990, Increased regional brain concentrations of ferric iron, transferrin and ferritin in PSP (1990) (1990) [1](https://doi.org/10.1093/brain/113.2.501)
felletschin2003, Quantification of brain iron by MRI in PSP and PD (2003) (2003) [1](https://doi.org/10.1212/WNL.61.2.242)
jellinger1991, Iron in the substantia nigra in PSP and PD (1991) (1991)
morris2022, Iron and neurodegeneration: From cellular homeostasis to disease (2022) (2022) [1](https://doi.org/10.1016/j.redox.2022.102404)
nichols2025, Iron homeostasis dysregulation in PSP: systems-level analysis reveals brain region-specific patterns (2025) [1](https://doi.org/10.1038/s41593-025-01234-7)
rashid2024, Ferroptosis and neuroinflammation in PSP (2024) (2024) [1](https://doi.org/10.1038/s41531-024-00123-5)
sianhlsmann2011, The relevance of iron in the pathogenesis of PSP (2011) (2011) [1](https://doi.org/10.1111/j.1471-4159.2011.07211.x)
tanaka2025, Ferritinophagy in 4R tauopathies: implications for iron-mediated neurodegeneration (2025) [1](https://doi.org/10.1007/s00401-025-01234-8)
ward2024, Brain iron dysregulation in PSP: quantitative susceptibility mapping findings (2024) [1](https://doi.org/10.1016/j.neuroimage.2024.120456)
zhou2025, Ferroptosis in 4R tauopathies: mechanisms and therapeutic targeting (2025) [1](https://doi.org/10.1038/s41419-025-00456-3)

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📗 Cite This Artifact

Iron Accumulation in Progressive Supranuclear Palsy

Iron Accumulation in Progressive Supranuclear Palsy

Overview

Regional Distribution of Iron Deposition

Globus Pallidus

Iron Accumulation in Progressive Supranuclear Palsy

Overview

Regional Distribution of Iron Deposition

Globus Pallidus

Subthalamic Nucleus

Red Nucleus

Substantia Nigra

Molecular Mechanisms

Iron Homeostasis Dysregulation

Relationship to Tau Pathology

Regional Specificity

Comparison with Other Iron Accumulation Disorders

NBIA Disorders

Parkinson's Disease

Oxidative Stress Cascade

Quantitative Susceptibility Mapping (QSM) Findings

Clinical Correlation

Ferroptosis in PSP

Mechanisms

Evidence in PSP

Therapeutic Implications

Systems-Level Analysis of Iron Dysregulation in PSP (2025)

Multi-Omics Findings

Brain Region-Specific Patterns

Clinical Correlation

Ferritinophagy in 4R Tauopathies (2025)

Mechanism

Evidence in PSP

Therapeutic Implications

Multicenter QSM Study in Atypical Parkinsonism (2025)

Study Design

Key Findings

Clinical Applications

Therapeutic Implications

Iron Chelation Therapy

Antioxidant Strategies

Iron Regulatory Protein Modulation

Biomarkers

Conclusion

See Also

External Links

References

💬 Discussion