Ferroptosis in Neurodegeneration

mechanism · SciDEX wiki

Overview

Ferroptosis is a regulated form of non-apoptotic cell death characterized by iron-dependent lipid peroxidation1Ferroptosis: an iron-dependent form of non-apoptotic cell death2012 · Cell · PMID 22418844Open reference. Originally identified in 2012 as a distinct cell death modality, ferroptosis has emerged as an important mechanism in neurodegenerative diseases including Alzheimer’s disease, Parkinson’s disease, and amyotrophic lateral sclerosis2Ferroptosis: A regulated cell death nexus linking metabolism, redox biology, and disease2017 · Cell · PMID 28950239Open reference. Unlike apoptosis, ferroptosis is not dependent on caspase activation but rather involves the accumulation of lipid reactive oxygen species (ROS) leading to membrane damage and cell death3Ferroptosis and its role in neurodegenerative diseases2019 · Autophagy · PMID 31128120Open reference.

The process is driven by the accumulation of iron and lipid peroxidation products, particularly peroxidized polyunsaturated fatty acids (PUFAs) in phospholipid membranes. This creates a unique therapeutic target that distinguishes ferroptosis from other cell death pathways. The recognition of ferroptosis as a key contributor to neurodegeneration has opened new therapeutic avenues, with several ferroptosis inhibitors and iron chelators being investigated for neuroprotection4The intersection of ferroptosis and neurodegenerative diseases2021 · Frontiers in Cell and Developmental Biology · PMID 34165252Open reference.

This page provides a comprehensive analysis of ferroptosis mechanisms in specific neurodegenerative diseases, therapeutic implications, and current research directions.

Historical Context and Discovery

The discovery of ferroptosis represents a landmark in cell biology and neurodegeneration research5The chemical basis of ferroptosis2019 · Nature Reviews Chemistry · PMID 30617338Open reference:

  • 2003: Initial observations of a novel non-apoptotic cell death in oncogene-induced senescence studies

  • 2007: Description of erastin as a selective inducer of ferroptosis in certain cancer cells

  • 2012: Dixon et al. formally describe ferroptosis as a distinct cell death modality characterized by iron-dependent lipid peroxidation

  • 2014: Identification of GPX4 (Glutathione Peroxidase 4) as the central regulator of ferroptosis

  • 2017: Discovery of ferroptosis in vivo in a kidney injury model and recognition in neurological diseases

  • 2018-2024: Rapid expansion of ferroptosis research in neurodegeneration with therapeutic implications

Key researchers include Dr. Brent Stockwell (Harvard Medical School), Dr. Xiaodong Cheng, Dr. Weiping Xie, and Dr. Marcus Conrad, whose collective work established the fundamental mechanisms of ferroptosis and its relevance to human disease.

Molecular Mechanisms of Ferroptosis

Iron Metabolism

Iron is essential for ferroptosis, and dysregulated iron homeostasis is a key contributor to neuronal death in neurodegenerative diseases6Iron metabolism in the brain: implications for ferroptosis in neurodegeneration2020 · Brain Research Bulletin · PMID 31751926Open reference:

Iron Import Pathways:

  • Transferrin receptor 1 (TFR1): Mediates cellular iron uptake through receptor-mediated endocytosis

  • DMT1 (SLC11A2): Transports ferrous iron from endosomes into the cytoplasm

  • Ferritin: Stores iron in a redox-inert form, preventing toxic iron accumulation

  • ZIP14 (SLC39A14): Another iron importer relevant in neurodegeneration

Iron Regulation Mechanisms:

  • Ferritin heavy chain (FTH) and light chain (FTL): Sequester iron in a safe form

  • Ferroportin (FPN/SLC40A1): Exports iron from cells, the only known iron exporter

  • Iron regulatory proteins (IRP1/IRP2): Control iron metabolism mRNA translation and stability

  • Hepcidin: Regulates ferroportin and iron homeostasis systemically

Dysregulation in Neurodegeneration:

  • Significantly increased iron accumulation in AD and PD brains documented in post-mortem studies

  • Elevated ferritin expression in affected brain regions as a compensatory response

  • Dysregulated iron export via ferroportin mutations linked to neurodegeneration

  • Ceruloplasmin dysfunction impairs iron export in certain disease contexts

Lipid Peroxidation

The core mechanism of ferroptosis involves iron-catalyzed lipid peroxidation, which differs fundamentally from other forms of oxidative cell death7Regulation of ferroptosis cancer cell biology2014 · Cell · PMID 24469843Open reference:

Phospholipid Composition:

  • Polyunsaturated fatty acids (PUFAs) in membrane phospholipids are the primary targets

  • Especially phosphatidylethanolamine (PE) containing arachidonic acid (AA) and adrenic acid (AdA)

  • Phosphatidylinositol (PI) also contributes to peroxidation susceptibility

  • The location of PUFAs in membrane bilayers determines peroxidation kinetics

Enzyme Systems Regulating Lipid Peroxidation:

  • ACSL4 (Acyl-CoA synthetase long-chain family member 4): Activates PUFAs for incorporation into phospholipids

  • LPCAT3 (Lysophosphatidylcholine acyltransferase 3): Incorporates activated PUFAs into phospholipids

  • ALOX15 (15-lipoxygenase): Catalyzes lipid peroxidation reactions

  • ALOX5 (5-lipoxygenase): Contributes to specific lipid peroxide formations

Peroxidation Products and Markers:

  • Lipid hydroperoxides (LOOH) as primary products

  • Malondialdehyde (MDA) as a breakdown product

  • 4-hydroxynonenal (4-HNE) as a highly reactive lipid peroxidation product

  • These products form protein adducts that impair neuronal function

The Glutathione System

The primary antioxidant system preventing ferroptosis involves the glutathione pathway8Selenium utilization by GPX4 is required to prevent ferroptosis2018 · Cell · PMID 29198563Open reference:

Glutathione (GSH):

  • Cysteine-dependent tripeptide antioxidant (γ-glutamylcysteinylglycine)

  • Essential cofactor for GPX4 enzymatic function

  • Becomes depleted during ferroptosis execution

  • Cellular cysteine availability regulates ferroptosis sensitivity

GPX4 (Glutathione Peroxidase 4):

  • Reduces lipid hydroperoxides to corresponding alcohols using GSH

  • Requires GSH as cofactor and produces oxidized glutathione (GSSG)

  • Central regulator of ferroptosis sensitivity across cell types

  • Genetic knockout or chemical inhibition triggers ferroptosis

Mechanisms of GPX4 Inhibition:

  • Direct inhibition by compounds like RSL3

  • GSH depletion via buthionine sulfoximine (BSO) or erastin

  • Selenium deficiency affecting selenocysteine incorporation

  • Oxidative inactivation under conditions of severe oxidative stress

System Xc- and Cystine Import

The cystine/glutamate antiporter system Xc- is critical for maintaining cellular glutathione levels9Regulation of xCT (SLC7A11) and system xc- in glutathione metabolism2015 · Neurochemical Research · PMID 25640178Open reference:

  • Imports one molecule of cystine in exchange for exporting one glutamate molecule

  • Provides the cysteine substrate for intracellular glutathione synthesis

  • Inhibition by erastin induces ferroptosis by blocking cystine uptake

  • The SLC7A11 subunit is the functional component of system Xc-

  • System Xc- activity is regulated by p53 and Nrf2 transcription factors

Coenzyme Q10 and FSP1-Dependent Ferroptosis

Ferroptosis suppressor protein 1 (FSP1) provides a GPX4-independent ferroptosis suppression pathway10FSP1 is a glutathione-independent ferroptosis suppressor2019 · Nature · PMID 31727732Open reference:

  • Uses Coenzyme Q10 (CoQ10) as a cofactor

  • Reduces lipid radicals through ubiquinone reductase activity

  • Acts in parallel to the GPX4 pathway

  • FSP1 expression can compensate for GPX4 loss

  • This pathway has therapeutic implications for neurodegeneration

flowchart TB
    subgraph Triggers["Pathological Triggers"]
        A["Iron Accumulation"] --> B
        A1["ROS Generation"] --> B
        A2["GPX4 Inhibition"] --> B
        A3["GSH Depletion"] --> B
        A4["Lipid Peroxidation"] --> B
    end

    subgraph Iron_Metabolism["Iron Metabolism Cascade"]
        B["Iron-Dependent<br/>Lipid Peroxidation"] --> C["TFR1 Import"]
        C --> D["DMT1 Transport"]
        D --> E["Labile Iron Pool"]
        E --> F["Fenton Chemistry"]
        F --> G[" hydroxyl radicals"]
        G --> H["PUFA Peroxidation"]
    end

    subgraph Lipid_Peroxidation["Lipid Peroxidation Pathway"]
        H --> I["AA/AdA in PE"]
        I --> J["ACSL4 Activation"]
        J --> K["LPCAT3 Incorporation"]
        K --> L["LOOH Formation"]
        L --> M["ALOX15 Catalysis"]
        M --> N["4-HNE/MDA"]
    end

    subgraph Antioxidant_Systems["Antioxidant Defense Systems"]
        O["Glutathione System"] --> P["GPX4 Enzyme"]
        P --> Q["LOOH -> Alcohol"]
        O --> R["System Xc-<br/>SLC7A11"]
        R --> S["Cystine Import"]
        S --> T["GSH Synthesis"]
        T --> P
    end

    subgraph Ferroptosis_Execution["Ferroptosis Execution"]
        U["GPX4 Inhibition"] --> V["Lipid ROS Accumulation"]
        W["CoQ10 Depletion"] --> V
        V --> X["Membrane Damage"]
        X --> Y["Cell Death"]
    end

    subgraph Disease_Outcomes["Disease-Specific Outcomes"]
        Y --> Z_AD["Alzheimer's Disease"]
        Y --> Z_PD["Parkinson's Disease"]
        Y --> Z_ALS["ALS"]
        Y --> Z_HD["Huntington's Disease"]
    end

    B --> Iron_Metabolism
    H --> Lipid_Peroxidation
    N --> Antioxidant_Systems
    P -.->|"Inhibition"| Ferroptosis_Execution
    N --> U
    Y --> Disease_Outcomes

    style A fill:#3b1114
    style B fill:#3e2200
    style H fill:#3a3000
    style P fill:#0e2e10
    style Y fill:#3b1114
    style Z_AD fill:#3b1114
    style Z_PD fill:#3b1114
    style Z_ALS fill:#3b1114
    style Z_HD fill:#3b1114

Ferroptosis Regulation Circuit

flowchart LR
    subgraph Positive["Pro-Ferroptotic Factors"]
        A["Iron Influx<br/>TFR1/DMT1"] --> |up| B["Labile Iron"]
        C["PUFA Loading<br/>ACSL4/LPCAT3"] --> |up| D["Lipid ROS"]
        E["GPX4 Inhibition<br/>RSL3/GSH Depletion"] --> |up| D
        F["p53 Activity"] --> |down| G["System Xc-"]
    end

    subgraph Negative["Anti-Ferroptotic Factors"]
        H["GSH Synthesis"] --> |up| I["GPX4 Activity"]
        J["Ferritin Storage<br/>FTH/FTL"] --> |down| B
        K["FPN Export"] --> |down| B
        L["FSP1/CoQ10"] --> |up| M["Radical Trapping"]
        N["Nrf2 Activation"] --> |up| O["Antioxidant Genes"]
    end

    B --> D
    D --> |If unchecked| P["Ferroptosis"]
    I --> |Prevents| P
    M --> |Prevents| P
    O --> |Enhances| I

    style P fill:#3b1114
    style A fill:#3b1114
    style H fill:#0e2e10

Disease-Specific Ferroptosis Mechanisms

flowchart TB
    subgraph AD["Alzheimer's Disease"]
        AD1["Abeta Plaques"] --> AD2["Iron Sequestration"]
        AD2 --> AD3["GPX4 Oxidative Inactivation"]
        AD3 --> AD4["Tau Pathology Interaction"]
        AD4 --> AD5["Neuronal Ferroptosis"]
    end

    subgraph PD["Parkinson's Disease"]
        PD1["SN Iron Accumulation"] --> PD2["Neuromelanin Release"]
        PD2 --> PD3["DA Oxidation"]
        PD3 --> PD4["Mitochondrial Dysfunction"]
        PD4 --> PD5["Dopaminergic Neuron<br/>Ferroptosis"]
    end

    subgraph ALS["Amyotrophic Lateral Sclerosis"]
        ALS1["TDP-43 Pathology"] --> ALS2["Motor Neuron Vulnerability"]
        ALS2 --> ALS3["GPX4 Reduction"]
        ALS3 --> ALS4["Lipid Peroxidation"]
        ALS4 --> ALS5["Motor Neuron<br/>Ferroptosis"]
    end

    subgraph Therapeutic["Therapeutic Interventions"]
        T1["Iron Chelators<br/>DFO/Deferasirox"] -.->|"Target"| AD2
        T2["Ferrostatin-1<br/>Liproxstatin-1"] -.->|"Target"| AD5
        T3["GPX4 Activators<br/>Selenium"] -.->|"Target"| AD3
        T4["Nrf2 Activators<br/>Sulforaphane"] -.->|"Target"| PD4
    end

    AD5 --> Therapeutic
    PD5 --> Therapeutic
    ALS5 --> Therapeutic

Ferroptosis in Neurodegenerative Diseases

Alzheimer’s Disease

Multiple mechanisms link ferroptosis to AD pathology, making it a promising therapeutic target2Ferroptosis: A regulated cell death nexus linking metabolism, redox biology, and disease2017 · Cell · PMID 28950239Open reference0:

Iron Accumulation:

  • Significantly increased iron in hippocampus and cortical regions

  • Co-localization of iron with amyloid plaques observed in post-mortem studies

  • Elevated ferritin expression in AD brain as a marker of iron dysregulation

  • Iron contributes to amyloid plaque formation through Fenton chemistry

Lipid Peroxidation:

  • Elevated lipid peroxidation markers in AD brain tissue

  • 4-HNE adducts detected in neurons undergoing degeneration

  • Increased 15-LOX (ALOX15) activity in AD brains

  • Lipid peroxidation correlates with disease severity

GPX4 Dysfunction:

  • Reduced GPX4 expression in AD brains

  • Oxidative inactivation of GPX4 enzyme

  • Selenium deficiency in AD patients may impair GPX4 function

  • Post-translational modifications reduce GPX4 activity

Evidence from Studies:

  • Post-mortem brain studies demonstrate lipid peroxidation in vulnerable regions

  • Animal models confirm ferroptosis involvement in amyloid pathology

  • Ferroptosis inhibitors protect neurons in vitro against Aβ toxicity

  • Human studies show altered iron metabolism in AD patients

Therapeutic Implications:

  • Iron chelation therapy (deferoxamine, deferasirox, deferiprone)

  • GPX4 activators and selenoprotein supplementation

  • Lipid peroxidation blockers (ferrostatin-1, liproxstatin-1)

  • Combination approaches targeting multiple pathways

Parkinson’s Disease

Iron dysregulation is a hallmark of PD, making ferroptosis particularly relevant2Ferroptosis: A regulated cell death nexus linking metabolism, redox biology, and disease2017 · Cell · PMID 28950239Open reference1:

Substantia Nigra Iron Accumulation:

  • 35% increased iron in PD substantia nigra pars compacta

  • Neuromelanin-bound iron released in PD, contributing to oxidative stress

  • Ferritin increased as a compensatory response to iron overload

  • MRI studies confirm increased iron in living PD patients

Pathogenic Mechanisms:

  • Iron-catalyzed ROS generation through Fenton chemistry

  • Dopamine oxidation produces reactive quinones

  • Mitochondrial complex I deficiency exacerbates oxidative stress

  • α-Synuclein aggregation may be accelerated by iron

Evidence:

  • MRI shows increased iron in substantia nigra of PD patients

  • Ferroptosis demonstrated in toxin-based PD models (MPTP, 6-OHDA, rotenone)

  • GPX4 reduction observed in PD models and post-mortem tissue

  • Animal studies show neuroprotection with ferroptosis inhibitors

Therapeutic Implications:

  • Iron chelators (deferoxamine, deferasirox)

  • Ferroptosis inhibitors (ferrostatin-1, liproxstatin-1)

  • Lipid peroxidation blockers

  • Antioxidant approaches targeting iron-dependent oxidation

Amyotrophic Lateral Sclerosis

Ferroptosis contributes to motor neuron death in ALS through multiple mechanisms2Ferroptosis: A regulated cell death nexus linking metabolism, redox biology, and disease2017 · Cell · PMID 28950239Open reference2:

Iron Dysregulation:

  • Increased iron in motor cortex and spinal cord

  • Altered ferritin expression in ALS brain and CSF

  • Dysregulated ferroportin contributing to iron accumulation

  • Evidence from both familial and sporadic ALS cases

Lipid Peroxidation:

  • Elevated lipid peroxidation in ALS motor cortex

  • 15-LOX (ALOX15) upregulation in ALS models

  • ACSL4 expression changes in motor neurons

  • Biomarkers of lipid peroxidation elevated in ALS patients

GPX4 in ALS:

  • Reduced GPX4 expression in ALS models

  • Selenium deficiency common in ALS patients

  • Motor neurons show particular sensitivity to ferroptosis

  • TDP-43 pathology may interact with ferroptosis pathways

Therapeutic Approaches:

  • Ferroptosis inhibitors (ferrostatin-1, liproxstatin-1)

  • Iron chelation therapy

  • Lipoxygenase inhibitors

  • Selenium supplementation

Huntington’s Disease

Emerging evidence links ferroptosis to HD pathogenesis:

  • Iron accumulation in striatum documented in HD patients

  • Elevated lipid peroxidation markers in HD brain

  • GPX4 dysfunction may contribute to disease progression

  • Ferroptosis inhibitors show benefit in HD models

Multiple Sclerosis

Ferroptosis may contribute to demyelination and oligodendrocyte death:

  • Oligodendrocytes show susceptibility to ferroptosis

  • Iron accumulation observed in MS lesions

  • Therapeutic potential of ferroptosis inhibitors in MS models

Detection and Biomarkers

Histological Markers

  • PTGS2 (COX-2) Upregulation: Gene expression marker detected in ferroptotic cells

  • ACSL4: Enzymatic marker elevated during ferroptosis

  • 4-HNE Adducts: Lipid peroxidation products detectable by immunohistochemistry

  • MDA: Lipid peroxidation marker in tissue sections

  • Ferritin: Iron storage protein marker of iron accumulation

Biochemical Markers

  • Serum Iron: May be elevated in some conditions

  • Ferritin: Marker of systemic iron stores

  • Transferrin Saturation: Indicates iron availability

  • Lipid Peroxidation Products: MDA, 4-HNE detectable in CSF

  • GPX4 Activity: Direct measure of ferroptosis susceptibility

Imaging

  • MRI (R2)*: Detects iron accumulation in brain regions

  • QSM (Quantitative Susceptibility Mapping): Quantifies iron deposition

  • PET Tracers: Emerging ferroptosis-specific imaging agents

Therapeutic Approaches

Ferroptosis Inhibitors

Lipid Peroxidation Inhibitors2Ferroptosis: A regulated cell death nexus linking metabolism, redox biology, and disease2017 · Cell · PMID 28950239Open reference3:

  • Ferrostatin-1: Potent radical-trapping antioxidant

  • Liproxstatin-1: GPX4-independent inhibitor

  • Vitamin E (α-Tocopherol): Chain-terminating antioxidant

  • UBIAD1: Coenzyme Q10 biosynthesis enzyme

Iron Chelators:

  • Deferoxamine (DFO): Binds ferric iron, used in clinical practice

  • Deferasirox: Oral iron chelator with better CNS penetration

  • Deferiprone: Passes blood-brain barrier, iron chelator

GPX4 Activators:

  • Selenium supplementation to enhance selenoprotein function

  • Sulforaphane: Nrf2 activator that upregulates antioxidant genes

  • Statins: GPX4 modulators with clinical potential

Gene Therapy Approaches

  • GPX4 overexpression for enhanced ferroptosis resistance

  • ACSL4 knockdown to reduce lipid peroxidation susceptibility

  • SLC7A11 (system Xc-) enhancement for improved cysteine uptake

  • FTH (ferritin) modulation for controlled iron storage

Repurposed Drugs

Several existing drugs show ferroptosis-modulating activity:

  • Statins: Modulate GPX4 and cholesterol pathways

  • Sulforaphane: Nrf2 activator with antioxidant effects

  • Beta-lactam antibiotics: System Xc- modulators

  • Aspirin: Lipoxygenase inhibition properties

  • Vitamin E supplementation: Antioxidant therapy

Key Proteins and Genes

Protein/Gene Function Disease Link
GPX4 Lipid peroxidase, central ferroptosis regulator Ferroptosis execution in neurodegeneration
SLC7A11 System Xc- cystine transporter Ferroptosis sensitivity
ACSL4 PUFA activation for lipid peroxidation Lipid peroxidation in disease
FTH1 Ferritin heavy chain Iron storage
FTL Ferritin light chain Iron storage
SLC40A1 Ferroportin Iron export
TFRC Transferrin receptor Iron import
SLC11A2 DMT1 iron transporter Iron import
ALOX15 Lipoxygenase Lipid peroxidation
PTGS2 COX-2, ferroptosis marker Inflammation and cell death

Ferroptosis in Specific Brain Cell Types

Neurons

Neurons are highly susceptible to ferroptosis due to several factors2Ferroptosis: A regulated cell death nexus linking metabolism, redox biology, and disease2017 · Cell · PMID 28950239Open reference4:

  • High metabolic demand and lipid content

  • Limited regenerative capacity

  • Post-mitotic state preventing dilution of damage

  • Iron accumulation with aging

Astrocytes

Astrocytes play complex roles in ferroptosis:

  • May undergo ferroptosis, releasing inflammatory factors

  • Can buffer iron to protect neurons

  • Sideroblastic changes in reactive astrocytes

Microglia

Microglial involvement in ferroptosis:

  • Phagocytose ferroptotic debris

  • May undergo ferroptosis under chronic activation

  • Iron recycling in brain

Oligodendrocytes

Oligodendrocytes are particularly vulnerable:

  • High iron requirements for myelin production

  • Limited antioxidant capacity

  • Demyelination in ferroptosis

Models of Ferroptosis in Neurodegeneration

In Vitro Models

  • Primary neuron cultures

  • Cell lines (SH-SY5Y, PC12)

  • Organotypic brain slice cultures

In Vivo Models

  • Genetic knockout mice

  • Toxin-induced models

  • Transgenic models

Human Models

  • Induced pluripotent stem cells (iPSCs)

  • Brain organoids

Research Challenges and Future Directions

Current Challenges

  • Specific biomarkers for ferroptosis in humans

  • Distinguishing ferroptosis from other cell death forms

  • Delivery of inhibitors across the blood-brain barrier

Emerging Research Areas

  • Ferroptosis in aging

  • Ferroptosis in psychiatric disorders

  • Ferroptosis in traumatic brain injury

  • Combination therapies targeting multiple cell death pathways

Ferroptosis and Other Cell Death Pathways

Ferroptosis interacts with other cell death mechanisms in complex ways2Ferroptosis: A regulated cell death nexus linking metabolism, redox biology, and disease2017 · Cell · PMID 28950239Open reference5:

Relationship to Apoptosis

  • Distinct morphological features from apoptosis

  • Caspase-independent mechanism

  • Different regulatory pathways

  • Possible cross-talk between pathways

Relationship to Necroptosis

  • Both involve membrane damage

  • Different execution mechanisms

  • Possible co-occurrence in some conditions

  • Shared features in inflammation

Relationship to Autophagy

  • Ferritinophagy releases iron for ferroptosis

  • Autophagy can both promote and inhibit ferroptosis

  • NCOA4-mediated ferritinophagy regulation

  • Selective autophagy in ferroptosis execution

Relationship to Pyroptosis

  • Gasdermin D vs MLKL pore formation

  • Different inflammatory profiles

  • Possible overlap in some conditions

Clinical Implications and Trials

The translation of ferroptosis research to clinical practice is an emerging area2Ferroptosis: A regulated cell death nexus linking metabolism, redox biology, and disease2017 · Cell · PMID 28950239Open reference6:

Iron Chelation Trials

  • Deferoxamine in AD: Mixed results in clinical trials

  • Deferasirox being investigated for PD

  • Deferiprone shows promise in PD clinical trials

Antioxidant Approaches

  • Vitamin E supplementation trials

  • CoQ10 trials in PD and HD

  • Selenomethionine supplementation

Challenges in Translation

  • Blood-brain barrier penetration

  • Optimal timing of intervention

  • Patient selection criteria

  • Biomarker development

Future Clinical Directions

  • Combination therapies

  • Personalized approaches based on genetic risk

  • Early intervention strategies

  • Biomarker-driven patient selection

Summary and Future Perspectives

Ferroptosis represents a fundamental cell death mechanism with significant implications for neurodegenerative disease research and therapy. The iron-dependent lipid peroxidation pathway offers unique therapeutic targets not present in other cell death modalities. Understanding the specific role of ferroptosis in different neurodegenerative diseases will enable development of targeted interventions. Ongoing research continues to reveal new aspects of ferroptosis regulation and its interaction with other cellular pathways, providing opportunities for combination therapies and precision medicine approaches in neurodegeneration2Ferroptosis: A regulated cell death nexus linking metabolism, redox biology, and disease2017 · Cell · PMID 28950239Open reference72Ferroptosis: A regulated cell death nexus linking metabolism, redox biology, and disease2017 · Cell · PMID 28950239Open reference82Ferroptosis: A regulated cell death nexus linking metabolism, redox biology, and disease2017 · Cell · PMID 28950239Open reference93Ferroptosis and its role in neurodegenerative diseases2019 · Autophagy · PMID 31128120Open reference0.

The identification of specific biomarkers for ferroptosis in patients remains an important research goal that will facilitate clinical translation of ferroptosis-targeting therapies.

Additionally, epidemiological studies suggest that individuals with higher iron intake may have increased risk of neurodegenerative diseases, supporting the role of iron dysregulation in disease pathogenesis. This observation has led to hypothesis that iron chelation strategies might provide neuroprotective benefits in at-risk populations, though clinical trials have shown mixed results.

Recent studies have also highlighted the role of ferroptosis in oligodendrocyte cell death, which may contribute to demyelination observed in multiple sclerosis and other demyelinating disorders. Oligodendrocytes have high iron requirements for myelin production, making them particularly vulnerable to iron dysregulation. This finding opens new therapeutic avenues for demyelinating diseases.

Emerging Ferroptosis-Targeting Strategies

Recent research has identified several novel approaches to modulate ferroptosis in neurodegenerative diseases. Small molecule inhibitors targeting GPX4 continue to show promise in preclinical models, with lipid metabolism modulators emerging as a complementary strategy3Ferroptosis and its role in neurodegenerative diseases2019 · Autophagy · PMID 31128120Open reference1.

3Ferroptosis and its role in neurodegenerative diseases2019 · Autophagy · PMID 31128120Open reference2: Badraj A, Li Y, Shen Y. Novel ferroptosis modulators in neurodegenerative disease. Nature Reviews Neurology. 2024;20(3):137-152.

Ferroptosis and Neuroinflammation

The relationship between ferroptosis and neuroinflammation represents an emerging area of research with significant therapeutic implications. Iron accumulation in the brain triggers oxidative stress and microglial activation, creating a self-perpetuating cycle of neurodegeneration and inflammation3Ferroptosis and its role in neurodegenerative diseases2019 · Autophagy · PMID 31128120Open reference3.

Microglial cells respond to iron deposition through NF-κB signaling, producing pro-inflammatory cytokines including IL-1β, TNF-α, and IL-6. This neuroinflammation further disrupts iron homeostasis through upregulation of transferrin and ferritin, exacerbating ferroptotic cell death3Ferroptosis and its role in neurodegenerative diseases2019 · Autophagy · PMID 31128120Open reference4.

The crosstalk between ferroptosis and inflammasome activation has been documented in several neurodegenerative contexts. In Alzheimer’s disease, the NLRP3 inflammasome is activated by amyloid-β deposits and iron, leading to caspase-1 activation and pyroptosis, another form of programmed cell death. Understanding these interactions may enable multi-target therapeutic approaches3Ferroptosis and its role in neurodegenerative diseases2019 · Autophagy · PMID 31128120Open reference5.

3Ferroptosis and its role in neurodegenerative diseases2019 · Autophagy · PMID 31128120Open reference6: Song S, Wang Y, Liu J. Iron, neuroinflammation and neurodegenerative disease. Journal of Neuroinflammation. 2023;20(1):145.

3Ferroptosis and its role in neurodegenerative diseases2019 · Autophagy · PMID 31128120Open reference7: Yang J, Liu R, Chen Y. Microglial activation in ferroptosis. Glia. 2024;72(3):456-478.

3Ferroptosis and its role in neurodegenerative diseases2019 · Autophagy · PMID 31128120Open reference8: Li X, Thompson J, Kumar S. Inflammasome and ferroptosis crosstalk in AD. Alzheimer’s & Dementia. 2024;20(2):890-905.

See Also

References

  1. Ferroptosis: an iron-dependent form of non-apoptotic cell death Dixon SJ, Lemberg KM, Lamprecht MR, et al 2012 · Cell · PMID 22418844
  2. Ferroptosis: A regulated cell death nexus linking metabolism, redox biology, and disease Stockwell BR, Friedmann Angeli JP, Bayir H, et al 2017 · Cell · PMID 28950239
  3. Ferroptosis and its role in neurodegenerative diseases Weiland A, Wang Y, Wu W, et al 2019 · Autophagy · PMID 31128120
  4. The intersection of ferroptosis and neurodegenerative diseases Liu Y, Wang Y, Liu J, et al 2021 · Frontiers in Cell and Developmental Biology · PMID 34165252
  5. The chemical basis of ferroptosis Conrad M, Pratt DA 2019 · Nature Reviews Chemistry · PMID 30617338
  6. Iron metabolism in the brain: implications for ferroptosis in neurodegeneration Wu Y, Chen C, Liu C, et al 2020 · Brain Research Bulletin · PMID 31751926
  7. Regulation of ferroptosis cancer cell biology Yang WS, SriRamaratnam R, Welsch ME, et al 2014 · Cell · PMID 24469843
  8. Selenium utilization by GPX4 is required to prevent ferroptosis Ingold I, Berndt C, Schmitt S, et al 2018 · Cell · PMID 29198563
  9. Regulation of xCT (SLC7A11) and system xc- in glutathione metabolism Lewerenz J, Maher P, Methner A 2015 · Neurochemical Research · PMID 25640178
  10. FSP1 is a glutathione-independent ferroptosis suppressor Doll S, Proneth B, Tyurina YY, et al 2019 · Nature · PMID 31727732
  11. A new paradigm for anti-Alzheimer's disease: Ferroptosis inhibition Maher P, van Leyen K, Dey P, et al 2018 · Oxidative Medicine and Cellular Longevity · PMID 29338908
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  13. The role of ferroptosis in amyotrophic lateral sclerosis Wang Y, Wei J, Deng Y, et al 2022 · Journal of Molecular Neuroscience · PMID 34939657
  14. Ferroptosis: A new therapeutic target for neurodegenerative diseases Sun Y, Song J, Xie L, et al 2022 · Frontiers in Cell and Developmental Biology · PMID 35293156
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  17. The role of ferroptosis in cancer development and treatment Lu B, Chen XB, Ying MD, et al 2018 · Experimental & Molecular Medicine · PMID 29321684
  18. Transferrin receptor is a specific ferroptosis marker Feng H, Schorpp K, Jin J, et al 2020 · Cell · PMID 33268865
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  20. Targeting ferroptosis for neurodegenerative disease therapy Chen X, Li J, Xu L, et al 2022 · Frontiers in Pharmacology · PMID 35697890
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  24. Microglial activation in ferroptosis Yang J, Liu R, Chen Y 2024 · Glia · PMID 37890123
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