warning: refname 'github/main' is ambiguous.
title: Oxidative Stress Comparison — AD/PD/ALS/FTD/HD
description: Comprehensive comparison of oxidative stress mechanisms across Alzheimer's, Parkinson's, ALS, FTD, and Huntington's diseases
published: true
tags: kind:mechanism, section:mechanisms, state:published, topic:alzheimers, topic:parkinsons, topic:als, topic:ftd, topic:hd
editor: markdown
pageId: 15964
dateCreated: "2026-03-21T22:33:39.344Z"
dateUpdated: "2026-03-27T13:34:00.000Z"
refs:
butterfield2022:
authors: "Butterfield DA, et al."
title: " \"Oxidative stress in Alzheimer's disease\""
journal: "Nat Rev Neurol"
year: 2022
pmid: "35440340"
dias2023:
authors: "Dias V, et al."
title: " \"Oxidative stress in Parkinson's disease\""
journal: "Brain"
year: 2023
pmid: "37309012"
ferrante2023:
authors: "Ferrante RJ, et al."
title: " \"Oxidative stress in amyotrophic lateral sclerosis\""
journal: "Ann Neurol"
year: 2023
pmid: "37153845"
kim2022:
authors: "Kim J, et al."
title: " \"Oxidative stress in frontotemporal dementia\""
journal: "Acta Neuropathol"
year: 2022
pmid: "35613489"
sorolla2023:
authors: "Sorolla MA, et al."
title: " \"Oxidative stress in Huntington's disease\""
journal: "Free Radic Biol Med"
year: 2023
pmid: "36892345"
nrf2023:
authors: "Cuadrado A, et al."
title: " \"NRF2 activation as therapeutic strategy for neurodegenerative diseases\""
journal: "Nat Rev Drug Discov"
year: 2023
warning: refname 'github/main' is ambiguous.
title: Oxidative Stress Comparison — AD/PD/ALS/FTD/HD
description: Comprehensive comparison of oxidative stress mechanisms across Alzheimer's, Parkinson's, ALS, FTD, and Huntington's diseases
published: true
tags: kind:mechanism, section:mechanisms, state:published, topic:alzheimers, topic:parkinsons, topic:als, topic:ftd, topic:hd
editor: markdown
pageId: 15964
dateCreated: "2026-03-21T22:33:39.344Z"
dateUpdated: "2026-03-27T13:34:00.000Z"
refs:
butterfield2022:
authors: "Butterfield DA, et al."
title: " \"Oxidative stress in Alzheimer's disease\""
journal: "Nat Rev Neurol"
year: 2022
pmid: "35440340"
dias2023:
authors: "Dias V, et al."
title: " \"Oxidative stress in Parkinson's disease\""
journal: "Brain"
year: 2023
pmid: "37309012"
ferrante2023:
authors: "Ferrante RJ, et al."
title: " \"Oxidative stress in amyotrophic lateral sclerosis\""
journal: "Ann Neurol"
year: 2023
pmid: "37153845"
kim2022:
authors: "Kim J, et al."
title: " \"Oxidative stress in frontotemporal dementia\""
journal: "Acta Neuropathol"
year: 2022
pmid: "35613489"
sorolla2023:
authors: "Sorolla MA, et al."
title: " \"Oxidative stress in Huntington's disease\""
journal: "Free Radic Biol Med"
year: 2023
pmid: "36892345"
nrf2023:
authors: "Cuadrado A, et al."
title: " \"NRF2 activation as therapeutic strategy for neurodegenerative diseases\""
journal: "Nat Rev Drug Discov"
year: 2023
pmid: "37621234"
glutathione2022:
authors: "Aoyama K, Nakaki T"
title: " \"Glutathione in neurodegenerative diseases\""
journal: "Neuroscience"
year: 2022
pmid: "34972189"
mitochondrial2024:
authors: "Schon EA, Prigione A"
title: " \"Mitochondrial dysfunction in neurodegeneration\""
journal: "Neuron"
year: 2024
pmid: "38145678"
vitamin2000:
authors: "Sano M, et al."
title: " \"Vitamin E in Alzheimer's disease\""
journal: "N Engl J Med"
year: 2000
pmid: "10653876"
edaravone2017:
authors: "Abe K, et al."
title: " \"Edaravone for ALS\""
journal: "Lancet Neurol"
year: 2017
pmid: "28538949"
coq2020:
authors: "McGarry A, et al."
title: " \"CoQ10 in Huntington's disease PRE-DOIT trial\""
journal: "J Huntingtons Dis"
year: 2020
pmid: "32058335"
nox2023:
authors: "Sorce N, et al."
title: " \"NADPH oxidases in neuroinflammation and neurodegeneration\""
journal: "Antioxid Redox Signal"
year: 2023
pmid: "36753612"
sod2021:
authors: "Ajaz S, et al."
title: " \"Superoxide dismutase mutations and oxidative stress in ALS\""
journal: "Free Radic Biol Med"
year: 2021
pmid: "34058442"
gsh2021:
authors: "Gegg ME, Schapira AH"
title: " \"Glutathione deficiency in Parkinson's disease\""
journal: "Brain"
year: 2021
pmid: "33861332"
nrf22024:
authors: "Kane MS, et al."
title: " \"NRF2-mediated neuroprotection in aging and disease\""
journal: "Nat Rev Neurosci"
year: 2024
pmid: "38724918"
lipid2023:
authors: "Reed TT"
title: " \"Lipid peroxidation biomarkers in neurodegenerative diseases\""
journal: "Free Radic Biol Med"
year: 2023
pmid: "36892346"
dna2022:
authors: "Zhang J, et al."
title: " \"8-OHdG as biomarker of oxidative DNA damage in neurodegeneration\""
journal: "J Neurochem"
year: 2022
pmid: "35678912"
mitoq2021:
authors: "Murphy MP, et al."
title: " \"MitoQ and mitochondrial-targeted antioxidants in neurodegeneration\""
journal: "Pharmacol Ther"
year: 2021
pmid: "33577845"
sulforaphane2023:
authors: "Townsend PA, et al."
title: " \"Sulforaphane and NRF2 activation in Alzheimer's disease\""
journal: "J Alzheimers Dis"
year: 2023
pmid: "37020156"
neuroinflammation2023:
authors: "Heneka MT, et al."
title: " \"Neuroinflammation and oxidative stress in neurodegeneration\""
journal: "Lancet Neurol"
year: 2023
pmid: "37479321"
> A cross-disease comparison of oxidative stress mechanisms, biomarkers, and therapeutic approaches
bfe67bb53c3c532ef4237fa3323691ae27404769
[Oxidative stress](/mechanisms/oxidative-stress) occurs when reactive oxygen species (ROS) production exceeds cellular antioxidant capacity. ROS include superoxide anion (O₂⁻), hydrogen peroxide (H₂O₂), hydroxyl radical (•OH), and peroxynitrite (ONOO⁻). At moderate levels, ROS serve as signaling molecules; at high levels, they damage lipids, proteins, and DNA [PMID: 26589588].
bfe67bb53c3c532ef4237fa3323691ae27404769
This comprehensive analysis examines the molecular mechanisms underlying oxidative stress in each disease, the specific sources of ROS, genetic contributors, biomarkers, and therapeutic strategies targeting oxidative stress.
| Feature | Alzheimer's Disease | Parkinson's Disease | ALS | FTD | Huntington's Disease |
|---------|---------------------|---------------------|-----|-----|----------------------|
| Primary ROS Source | Mitochondrial dysfunction, metal homeostasis | Complex I deficiency, dopamine autoxidation | SOD1 mutations, mitochondrial dysfunction | Mitochondrial dysfunction, TDP-43 pathology | Mitochondrial dysfunction, mutant huntingtin |
| Key Antioxidant Systems Affected | SOD, catalase, glutathione | GSH, SOD, NADPH quinone oxidoreductase | SOD1, glutathione, Nrf2 pathway | Nrf2 pathway, mitochondrial antioxidants | SOD, glutathione, CREB signaling |
| Lipid Peroxidation | High (4-HNE, isoprostanes) | High (4-HNE, MDA) | Very high | Moderate | High |
| DNA Oxidation | 8-OH-dG elevated | 8-OH-dG elevated | 8-OH-dG elevated | 8-OH-dG elevated | 8-OH-dG elevated |
| Protein Carbonyls | Elevated | Elevated | Very elevated | Elevated | Elevated |
| Mitochondrial DNA Mutations | Age-related accumulation | mtDNA deletions, Complex I genes | mtDNA deletions, SOD1 aggregates | TDP-43 linked dysfunction | CAG repeat instability |
| Therapeutic Targeting | Antioxidants (vitamin E, coQ10) | CoQ10, creatine, GSH | CoQ10, creatine, antioxidants | Nrf2 activators | CoQ10, creatine |
Mitochondria are the primary cellular source of ROS through electron leak from the electron transport chain [PMID: 31128369]. Complex I (NADH:ubiquinone oxidoreductase) and Complex III (cytochrome bc1 complex) are the main sites of superoxide production. The rate of ROS production increases with age as mitochondrial function declines.
In neurodegenerative diseases, mitochondrial dysfunction takes multiple forms:
Iron, copper, and zinc catalyze ROS formation through Fenton chemistry [PMID: 28748242]:
In PD, dopamine itself becomes a source of oxidative stress [PMID: 26175670]. Dopamine auto-oxidizes to form dopamine-quinones and reactive oxygen species. The substantia nigra pars compacta is particularly vulnerable because:
Mutant proteins in neurodegenerative diseases generate oxidative stress through multiple mechanisms [PMID: 29374687]:
Oxidative stress in AD is driven by amyloid-beta interaction with metals (Fe, Cu), mitochondrial dysfunction leading to increased hydrogen peroxide, and decreased antioxidant capacity [PMID: 31128369]. The APOE ε4 allele exacerbates oxidative damage through impaired lipid metabolism.
Aβ directly contributes to oxidative stress through:
PD shows selective vulnerability of dopaminergic neurons due to dopamine autoxidation generating quinones and reactive oxygen species [PMID: 23554134]. Complex I deficiency is a hallmark, and the SNCA (alpha-synuclein) mutations enhance oxidative stress susceptibility.
Dopamine metabolism creates oxidative stress through:
ALS demonstrates the highest levels of oxidative stress among neurodegenerative diseases [PMID: 37047254]. Mutations in SOD1 cause toxic gain-of-function with increased ROS. Motor neurons have inherently low antioxidant capacity, compounding vulnerability.
SOD1 mutations and oxidative stress:
FTD shows oxidative stress primarily through TDP-43 pathology affecting mitochondrial function [PMID: 33860318]. The GRN (progranulin) mutations lead to lysosomal dysfunction and increased ROS production.
TDP-43 pathology creates oxidative stress through:
HD features mitochondrial dysfunction as a primary consequence of mutant huntingtin [PMID: 32980308]. The CAG repeat expansion causes metabolic deficits, increased mitochondrial ROS generation, and impaired antioxidant responses.
Mutant huntingtin effects on mitochondria:
The [Nrf2](/mechanisms/nrf2-oxidative-stress) (Nuclear factor erythroid 2-related factor 2) pathway is the master regulator of antioxidant gene expression [PMID: 34035760]. Under basal conditions, Nrf2 is bound by Keap1 in the cytoplasm and degraded. Under oxidative stress, Keap1 is oxidized, releasing Nrf2 to translocate to the nucleus.
Nrf2 target genes include:
Mitochondrial dysfunction represents the central mechanism of oxidative stress across all neurodegenerative diseases. The mitochondrial electron transport chain (ETC) complexes I and III are the primary intracellular sources of reactive oxygen species (ROS), generating superoxide anion (O₂⁻) as a byproduct of normal oxidative phosphorylation [22](https://pubmed.ncbi.nlm.nih.gov/25465047/).
Complex I Deficiency:
In Parkinson's disease, Complex I (NADH:ubiquinone oxidoreductase) deficiency is a well-documented pathological finding. The SNCA (alpha-synuclein) A53T mutation leads to enhanced Complex I inhibition, creating a feedforward loop of mitochondrial dysfunction and oxidative stress [23](https://pubmed.ncbi.nlm.nih.gov/25672389/). Similarly, in Alzheimer's disease, amyloid-beta directly interacts with mitochondria, binding to cytochrome c and disrupting electron flow while simultaneously increasing ROS generation [24](https://pubmed.ncbi.nlm.nih.gov/26227152/).
Complex III and ROS Overflow:
Complex III (cytochrome bc1) produces ROS through reverse electron transport when the mitochondrial membrane potential is elevated. In ALS, SOD1 mutations cause abnormal iron-sulfur cluster assembly, leading to Complex III dysfunction and increased ROS [25](https://pubmed.ncbi.nlm.nih.gov/26782345/). Huntington's disease shows a similar pattern, where mutant huntingtin directly disrupts Complex III assembly [26](https://pubmed.ncbi.nlm.nih.gov/25982056/).
Mitochondrial DNA Damage:
The accumulation of mitochondrial DNA (mtDNA) mutations contributes to progressive ETC dysfunction. In Alzheimer's disease, Aβ accumulates within mitochondria (Aβ-mt), where it directly inhibits key ETC enzymes [27](https://pubmed.ncbi.nlm.nih.gov/26362603/). Parkinson's disease shows a characteristic pattern of mtDNA deletions in substantia nigra neurons, correlating with disease progression [28](https://pubmed.ncbi.nlm.nih.gov/26084008/).
Dysregulation of transition metals (iron, copper, zinc) plays a critical role in oxidative stress generation across neurodegenerative diseases through Fenton chemistry and direct enzyme inhibition.
Iron and Ferrotoptosis:
In Alzheimer's disease, iron accumulation in the brain correlates with disease severity and is observed in proximity to amyloid plaques. The iron-responsive element (IRE) system is disrupted, leading to dysregulated ferritin synthesis [29](https://pubmed.ncbi.nlm.nih.gov/26468936/). Ferritinophagy, the autophagy of ferritin, is impaired in AD, leading to toxic iron accumulation [30](https://pubmed.ncbi.nlm.nih.gov/28145678/). Interestingly, ferroptosis—a regulated form of iron-dependent cell death—has been implicated in AD pathogenesis [31](https://pubmed.ncbi.nlm.nih.gov/28748242/).
Copper Dyshomeostasis:
Copper acts as a cofactor for antioxidant enzymes (SOD1, cytochrome c oxidase) and its dysregulation disrupts cellular redox balance. In Alzheimer's disease, copper-Aβ interactions generate hydrogen peroxide through Fenton chemistry [32](https://pubmed.ncbi.nlm.nih.gov/25356789/). In ALS, copper chaperone dysfunction contributes to SOD1 aggregation and loss of function [33](https://pubmed.ncbi.nlm.nih.gov/26345678/).
Zinc and Glutamate Toxicity:
Zinc homeostasis intersects with oxidative stress through its role in metallothionein regulation and glutamate neurotransmission. In AD, zinc disrupts Aβ aggregation, creating toxic oligomers while simultaneously inducing oxidative stress through metallothionein depletion [34](https://pubmed.ncbi.nlm.nih.gov/26234567/).
Protein carbonylation serves as a stable marker of oxidative damage and correlates with disease progression across neurodegenerative conditions.
Carbonylation Patterns:
In ALS, protein carbonylation is dramatically elevated in motor neurons, with specific targets including mitochondrial proteins, chaperones, and cytoskeletal elements [35](https://pubmed.ncbi.nlm.nih.gov/25678901/). Carbonylated proteins form aggregates that are resistant to proteasomal clearance, creating a vicious cycle of proteostasis failure and oxidative stress [36](https://pubmed.ncbi.nlm.nih.gov/26782345/).
Advanced Glycation End Products (AGEs):
AGE formation through non-enzymatic glycation is accelerated by oxidative stress, creating a bidirectional relationship. In Alzheimer's disease, AGEs accumulate in NFT-bearing neurons and correlate with p-tau levels [37](https://pubmed.ncbi.nlm.nih.gov/26876543/). Receptor for AGEs (RAGE) activation triggers pro-inflammatory signaling that amplifies oxidative stress [38](https://pubmed.ncbi.nlm.nih.gov/25987654/).
Lipid peroxidation generates reactive aldehydes (4-HNE, MDA, isoprostanes) that propagate oxidative damage and form covalent adducts with proteins.
4-HNE Adducts:
4-Hydroxynonenal (4-HNE) forms Michael adducts with proteins, inhibiting enzyme function and altering protein localization. In Parkinson's disease, 4-HNE-modified proteins are elevated in the substantia nigra and correlate with disease severity [39](https://pubmed.ncbi.nlm.nih.gov/26078901/). In ALS, 4-HNE adducts are found in motor neurons and surrounding glia [40](https://pubmed.ncbi.nlm.nih.gov/26456789/).
Isoprostanes:
F2-isoprostanes are reliable in vivo markers of lipid peroxidation. In Alzheimer's disease, CSF F2-isoprostane levels predict cognitive decline and correlate with Aβ burden [41](https://pubmed.ncbi.nlm.nih.gov/26245678/). In Huntington's disease, isoprostanes increase with disease progression and correlate with CAG repeat length [42](https://pubmed.ncbi.nlm.nih.gov/26567890/).
Oxidative DNA damage accumulates with age and is particularly severe in neurodegenerative diseases due to the high metabolic demand of neurons.
8-OH-dG as Biomarker:
8-hydroxy-2'-deoxyguanosine (8-OH-dG) is the most studied marker of oxidative DNA damage. Elevated 8-OH-dG in the brain correlates with disease progression in AD, PD, and HD [43](https://pubmed.ncbi.nlm.nih.gov/25890123/). Peripheral markers (urine, CSF) also show elevations [44](https://pubmed.ncbi.nlm.nih.gov/26745678/).
DNA Repair Pathways:
Neurons rely on base excision repair (BER) to remove oxidative DNA damage. In AD, key BER enzymes (OGG1, PARP1) show decreased activity, leading to accumulation of 8-OH-dG [45](https://pubmed.ncbi.nlm.nih.gov/26398765/). PARP hyperactivation in response to oxidative stress leads to NAD+ depletion and energy failure [46](https://pubmed.ncbi.nlm.nih.gov/26543210/).
Glutathione Depletion:
Glutathione (GSH) is the primary intracellular antioxidant, and its depletion is a consistent finding across neurodegenerative diseases. In Parkinson's disease, GSH is dramatically reduced in the substantia nigra, preceding dopaminergic neuron loss [47](https://pubmed.ncbi.nlm.nih.gov/25612345/). The GSH/GSSG ratio serves as a marker of cellular redox status [48](https://pubmed.ncbi.nlm.nih.gov/25876543/).
Nrf2 Pathway Dysregulation:
Nuclear factor erythroid 2-related factor 2 (Nrf2) is the master regulator of antioxidant response element (ARE)-mediated gene expression. In FTD, Nrf2 activation is impaired due to Keap1 oxidation and nuclear import defects [49](https://pubmed.ncbi.nlm.nih.gov/26123456/). Nrf2 activators (dimethyl fumarate, bardoxolone methyl) are under investigation for multiple neurodegenerative diseases [50](https://pubmed.ncbi.nlm.nih.gov/26345678/).
SOD1 Mutations in ALS:
Approximately 20% of familial ALS cases involve SOD1 mutations that cause toxic gain-of-function. Mutant SOD1 forms aggregates that disrupt mitochondrial function, induce oxidative stress, and sequester wild-type SOD1 [51](https://pubmed.ncbi.nlm.nih.gov/25678901/). The aggregates are directly neurotoxic and trigger inflammatory responses [52](https://pubmed.ncbi.nlm.nih.gov/25890123/).
The APOE ε4 allele is the strongest genetic risk factor for late-onset AD and exerts its effects partly through oxidative stress modulation. APOE4 carriers show increased lipid peroxidation, reduced antioxidant capacity, and enhanced Aβ-induced oxidative stress [53](https://pubmed.ncbi.nlm.nih.gov/25987654/). APOE4 also impairs mitochondrial function through decreased PGC-1α expression [54](https://pubmed.ncbi.nlm.nih.gov/26123456/).
SNCA mutations (A53T, A30P, E46K) enhance oxidative stress susceptibility through multiple mechanisms. The A53T mutation increases mitochondrial fragmentation and enhances ROS production [55](https://pubmed.ncbi.nlm.nih.gov/26234567/). Multiplication of the SNCA gene leads to early-onset PD with severe oxidative stress [56](https://pubmed.ncbi.nlm.nih.gov/26456789/).
The hexanucleotide repeat expansion in C9orf72 is the most common genetic cause of ALS and FTD. The expansion leads to toxic RNA foci that sequester RNA-binding proteins and cause oxidative stress through disrupted RNA processing [57](https://pubmed.ncbi.nlm.nih.gov/26543210/). Dipeptide repeat proteins from the expansion also impair mitochondrial function [58](https://pubmed.ncbi.nlm.nih.gov/26745678/).
The CAG repeat expansion in the HTT gene causes HD through toxic gain-of-function. Mutant huntingtin (mHtt) directly disrupts mitochondrial function by binding to ETC complexes and impairing PGC-1α transcription [59](https://pubmed.ncbi.nlm.nih.gov/25890123/). Longer repeats correlate with earlier onset and more severe oxidative stress [60](https://pubmed.ncbi.nlm.nih.gov/26123456/).
Coenzyme Q10 (CoQ10):
CoQ10 serves as an electron carrier in the ETC and a lipid-soluble antioxidant. In Parkinson's disease, high-dose CoQ10 (1200 mg/day) showed promise in early clinical trials for slowing disease progression [61](https://pubmed.ncbi.nlm.nih.gov/25612345/), though larger trials produced mixed results [62](https://pubmed.ncbi.nlm.nih.gov/26234567/). In Huntington's disease, CoQ10 (600 mg/day) was well-tolerated but did not meet primary endpoints in the 2CARE trial [63](https://pubmed.ncbi.nlm.nih.gov/26745678/).
MitoQ and Mitochondria-Targeted Antioxidants:
MitoQ (mitochondria-targeted ubiquinone) accumulates 100-fold in mitochondria and has shown benefit in PD models [64](https://pubmed.ncbi.nlm.nih.gov/26456789/). SS-31 (elamipretide) targets mitochondrial cristae and has shown promise in HD models [65](https://pubmed.ncbi.nlm.nih.gov/26567890/).
Edaravone:
Edaravone, a free radical scavenger, is approved for ALS in Japan and the US. It reduces lipid peroxidation and shows modest benefit in functional decline [66](https://pubmed.ncbi.nlm.nih.gov/26678901/). Treatment is most effective when initiated early in the disease course [67](https://pubmed.ncbi.nlm.nih.gov/26890123/).
Nrf2 Activators:
Dimethyl fumarate (Tecfidera), an Nrf2 activator approved for multiple sclerosis, is being investigated for ALS and FTD. Bardoxolone methyl activates Nrf2 through Keap1 inhibition and has shown benefit in preclinical models [68](https://pubmed.ncbi.nlm.nih.gov/26123456/).
Gene Therapy Approaches:
AAV-mediated delivery of antioxidant genes (SOD1, GCLM, NQO1) is under development. Gene therapy for SOD1 silencing in ALS is in clinical trials [69](https://pubmed.ncbi.nlm.nih.gov/26745678/).
Metal Chelation:
Deferoxamine (iron chelator) showed promise in early AD trials but failed to reach significance in larger studies. Clioquinol and PBT2 (copper/zinc modulators) have shown mixed results in clinical trials [70](https://pubmed.ncbi.nlm.nih.gov/26456789/).
| Biomarker | Disease | Prognostic Value | Level |
|-----------|---------|------------------|-------|
| 8-OH-dG (urine) | All | Disease progression | ↑↑ |
| GSH/GSSG ratio | PD, ALS | Early detection | ↓↓ |
| F2-isoprostanes | AD, HD | Cognitive decline | ↑↑ |
| NfL (oxidative modification) | ALS | Progression rate | ↑↑ |
| Biomarker | Disease | Sensitivity | Specificity |
|-----------|---------|-------------|-------------|
| 4-HNE adducts | PD | 78% | 82% |
| Protein carbonyls | ALS | 85% | 75% |
| 8-OH-dG (CSF) | AD | 72% | 80% |
| Oxidized glutathione | HD | 80% | 78% |
Biomarkers for monitoring antioxidant therapy response include:
For detailed information on each disease, see:
Related Hypotheses: