Submitted:
10 February 2026
Posted:
11 February 2026
You are already at the latest version
Abstract
Keywords:
1. Introduction
2. Ferroptosis Mechanistic Drivers
2.1. Oxidative Stress and Lipid Peroxidation
2.2. Antioxidant Defense System
2.3. Iron Dysregulation and Labile Iron Pool
3. Ferroptosis Vulnerability Factors
4. Ferroptosis in Neurodegenerative Diseases
4.1. Parkinson’s Disease
4.2. Alzheimer’s Disease
4.3. Huntington’s Disease
4.4. Amyotrophic Lateral Sclerosis
4.5. Other Diseases
5. In Vivo Detection of Ferroptosis
6. Therapeutic Strategies for Neurodegenerative Diseases
7. Ferroptosis-Targeted Neuroprotection
8. Nutritional Neuroroprotection Against Ferroptosis
8.1. Multivitamins
8.2. Jucara Fruit Extract
8.3. Flavonoids
9. Future Technologies and Challenges
10. Conclusion
Author Contributions
Funding
Institutional Review Board Statement
Informed Consent Statement
Data Availability Statement
Conflicts of Interest
References
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| Mechanisms | Purpose | Method Examples | Role of Action | References |
|---|---|---|---|---|
| Dopamine-based therapies | Inhibitor | Levodopa, a dopamine receptor agonist | In PD, these drugs can cross the BBB, facilitate the removal of excess iron from the brain, and stabilize GPX4. | [91] |
| TfR 1 regulators | Inhibitor | Hepcidin agonist | In AD, regulating TfR 1 mediates cellular iron uptake and maintains iron homeostasis in neuronal cells. | [110] |
| Antioxidants | Inhibitor | Fer-1, Lip-1 |
It targets lipid peroxidation and slows cognitive decline in patients with mild-to-moderate AD. It blocks ROS and effectively fixes AB-induced neuronal death | [98] |
| ROS free radicals | Inhibitor | Edaravone | In ALS patients, it reduces motor neuron damage and inhibits ferroptosis. | [105] |
| Iron Chelators | Inhibitor | DFP, DFO, DFE |
In PD, it protects against neuronal injury through inhibiting ferroptosis. In AD, DFO inhibits erastin-induced ROS accumulation. In ALS, it is shown to improve motor neuron survival and restore motor function. In HD, IV administration of DFO shown to relieve symptoms in mouse models. |
[102,103,107] |
| Vitamin E | Inhibitor | A-tocopherol | It targets lipid peroxidation and slows cognitive decline in patients with mild-to-moderate AD. It destroys the chain reaction of automatic oxidation. | [99] |
| Nitroxides | Inhibitor | NOX2 mediated ROS, Iron (II) citrate |
In neurogenerative diseases, nitroxides can cross the BBB and target lipid peroxidation. In AD, nitroxides positively induce neuroplasticity and neuroprotection. |
[23] |
| Selenium | Inhibitor | Selenocysteine, Tat SelPep | It acts as the active site of GPX4 and can cross the BBB to help protect against ferroptosis. | [100] |
| Zileuton | Inhibitor | 5-lipoxygenase (LOX) | It protects cells from lipid peroxidation by down-regulating LOX. | [93] |
| Erastin | Inducer | System Xc- | It mediates ferroptosis via inhibiting system Xc-. | [116] |
| Glutamate | Inducer | cystine | It mediates ferroptosis through cystine uptake inhibition of system Xc-. | [16] |
| Sulfasalazine | Inducer | System Xc- | It mediates ferroptosis via inhibiting system Xc-. | [16] |
| Sorafenin | Inducer | cystine | It mediates ferroptosis through cystine uptake inhibition of system Xc-. | [14] |
| RSL3 | Inducer | Selenocysteine | It blocks the activity of GSH and GPX4 at the active site selenocysteine. | [8] |
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