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Oxidatively Damaged Neurons
Oxidatively Damaged Neurons
<table class="infobox infobox-celltype">
<tr>
<th class="infobox-header" colspan="2">Oxidatively Damaged Neurons</th>
</tr>
<tr> [@bedard2007]
<td class="label">Lineage</td> [@pacher2007]
<td>Neuron > Oxidatively Damaged</td> [@rikans1997]
</tr> [@valentine2004]
<tr> [@dringen2000]
<td class="label">Markers</td> [@schrader2006]
<td>4-HNE, 8-OHdG, Carbonyls, 3-NT, 8-oxoguanine</td> [@holmgren2000]
</tr> [@stadtman2000]
<tr> [@greenacre2001]
<td class="label">Brain Regions</td> [@vogt1995]
<td>Substantia Nigra, Hippocampus, Cerebral Cortex, Basal Forebrain</td> [@dalledonne2003]
</tr> [@esterbauer1991]
<tr> [@del2005]
<td class="label">Disease Relevance</td> [@morrow2000]
<td>Alzheimer's Disease, Parkinson's Disease, Huntington's Disease, Stroke, ALS</td> [@terman2004]
</tr> [@kino2005]
</table> [@alano2010]
Oxidatively Damaged Neurons
Overview
...Oxidatively Damaged Neurons
<table class="infobox infobox-celltype">
<tr>
<th class="infobox-header" colspan="2">Oxidatively Damaged Neurons</th>
</tr>
<tr> [@bedard2007]
<td class="label">Lineage</td> [@pacher2007]
<td>Neuron > Oxidatively Damaged</td> [@rikans1997]
</tr> [@valentine2004]
<tr> [@dringen2000]
<td class="label">Markers</td> [@schrader2006]
<td>4-HNE, 8-OHdG, Carbonyls, 3-NT, 8-oxoguanine</td> [@holmgren2000]
</tr> [@stadtman2000]
<tr> [@greenacre2001]
<td class="label">Brain Regions</td> [@vogt1995]
<td>Substantia Nigra, Hippocampus, Cerebral Cortex, Basal Forebrain</td> [@dalledonne2003]
</tr> [@esterbauer1991]
<tr> [@del2005]
<td class="label">Disease Relevance</td> [@morrow2000]
<td>Alzheimer's Disease, Parkinson's Disease, Huntington's Disease, Stroke, ALS</td> [@terman2004]
</tr> [@kino2005]
</table> [@alano2010]
Oxidatively Damaged Neurons
Overview
Oxidatively Damaged [Neurons](/entities/neurons) plays an important role in the study of neurodegenerative diseases. This page provides comprehensive information about this topic, including its mechanisms, significance in disease processes, and therapeutic implications. [@von2002]
Introduction
Oxidatively damaged neurons represent a critical pathological state in which [reactive oxygen species](/entities/reactive-oxygen-species) (ROS) overwhelm cellular antioxidant defenses, leading to covalent modifications of proteins, lipids, and nucleic acids. This oxidative damage disrupts neuronal function through multiple mechanisms including enzyme inactivation, membrane lipid peroxidation, DNA damage, and disruption of cellular signaling pathways [1]. The brain is particularly vulnerable to oxidative stress due to its high metabolic rate, elevated oxygen consumption, and relatively limited antioxidant capacity compared to other organs [2]. [@wallace2005]
Unlike acute oxidative insults that cause rapid necrotic cell death, oxidatively damaged neurons often undergo progressive degeneration characterized by chronic oxidative stress, mitochondrial dysfunction, and eventual apoptotic or necrotic cell death. Understanding the mechanisms of oxidative damage and developing neuroprotective strategies targeting these pathways remains a major focus of neurodegeneration research [3]. [@lenaz2002]
Molecular Mechanisms
Reactive Oxygen Species Sources
- Mitochondrial electron transport chain: Complex I and III leak electrons forming superoxide [4]
- NADPH oxidases: Activation produces ROS in response to various stimuli [5]
- Xanthine oxidase: Uric acid catabolism generates hydrogen peroxide [6]
- Cytochrome P450 enzymes: Xenobiotic metabolism produces ROS as byproducts [7]
Antioxidant System Impairment
- Superoxide dismutase (SOD) dysfunction: Mutations and aggregation impair ROS scavenging [8]
- Glutathione depletion: Reduced GSH levels compromise cellular redox buffer [9]
- Catalase impairment: Reduced hydrogen peroxide detoxification [10]
- Thioredoxin system disruption: Impaired protein disulfide reduction [11]
Protein Oxidation
- Carbonyl formation: Metal-catalyzed oxidation of amino acid side chains [12]
- 3-Nitrotyrosine: Peroxynitrite-mediated tyrosine nitration [13]
- Methionine oxidation: Formation of methionine sulfoxide [14]
- Protein aggregation: Oxidized proteins form toxic oligomers [15]
Lipid Peroxidation
- 4-HNE formation: Reactive aldehyde from omega-6 fatty acid oxidation [16]
- Malondialdehyde (MDA): End product of lipid peroxidation [17]
- F2-isoprostanes: Prostaglandin-like compounds from arachidonic acid [18]
- Lipofuscin accumulation: Autofluorescence of oxidized lipids [19]
DNA Damage
- 8-oxoguanine: Most common oxidative DNA lesion [20]
- Single-strand breaks: PARP activation signals DNA damage [21]
- Telomere attrition: Oxidative stress accelerates aging [22]
- Mitochondrial DNA mutations: Accumulation impairs function [23]
Cellular Manifestations
Mitochondrial Dysfunction
- Electron transport chain inhibition: Oxidative damage to complexes [24]
- Mitochondrial DNA damage: Impairs encoded proteins [25]
- Permeability transition: Pore opening releases cytochrome c [26]
- Fusion/fission imbalance: Disrupted mitochondrial dynamics [27]
Membrane Damage
- Lipid raft disruption: Altered signal transduction [28]
- Ion channel oxidation: Impaired neuronal excitability [29]
- Receptor dysfunction: Oxidative modification of neurotransmitter receptors [30]
- Synaptic vesicle damage: Impaired neurotransmitter release [31]
ER Stress
- [Unfolded protein response](/entities/unfolded-protein-response): CHOP-mediated [apoptosis](/entities/apoptosis) [32]
- Calcium dysregulation: ER calcium release increases oxidative stress [33]
- Protein misfolding: Oxidized proteins fail to fold properly [34]
Lysosomal Damage
- [Autophagy](/entities/autophagy) impairment: Damaged lysosomes leak enzymes [35]
- Lipofuscin accumulation: Non-degradable material [36]
- [Cathepsin release: Initiates apoptotic cascade [37]
Role in Alzheimer's Disease
Amyloid-Beta Oxidative Stress
- Metal binding: Cu/Zn binding to [Aβ](/proteins/amyloid-beta) generates H2O2 [38]
- Mitochondrial dysfunction: Aβ localizes to mitochondria [39]
- NADPH oxidase activation: Microglial ROS production [40]
Tau-Mediated Oxidative Damage
- GSK3β activation: Kinase increases ROS production [41]
- Mitochondrial trafficking disruption: Energy deficit [42]
- Metabolic impairment: Altered glucose metabolism [43]
Regional Vulnerability
- [Hippocampus](/brain-regions/hippocampus): High metabolic demand increases ROS [44]
- Substantia nigra: Neuromelanin complexes with iron [45]
- [Cortex](/brain-regions/cortex): Variable susceptibility to oxidative damage [46]
Role in Parkinson's Disease
Mitochondrial Complex I Deficiency
- Complex I inhibition: Rotenone and MPTP models [47]
- PINK1 mutations: Impaired mitophagy [48]
- Parkin dysfunction: Defective mitochondrial quality control [49]
Neuromelanin Oxidation
- Iron accumulation: Fenton chemistry generates ROS [50]
- Dopamine oxidation: Auto-oxidation produces quinones [51]
- Lipid peroxidation: Substantia nigra vulnerability [52]
Neuroinflammation
- Microglial activation: NADPH oxidase ROS production [53]
- Cytokine release: TNF-α and IL-1β increase oxidative stress [54]
- [Peripheral inflammation: Systemic oxidative stress [55]
Role in Huntington's Disease
Mutant Huntingtin Effects
- Transcriptional dysregulation: Mitochondrial gene expression [56]
- Energy deficit: Creatine and ATP reductions [57]
- Axonal transport defects: Mitochondrial trafficking impairment [58]
Oxidative Damage Markers
- Elevated 8-OHdG: DNA oxidation in patient brains [59]
- Increased 4-HNE: Lipid peroxidation products [60]
- Protein carbonyls: Widespread protein oxidation [61]
Therapeutic Approaches
Antioxidant Therapies
- Vitamin E: Lipid-soluble antioxidant [62]
- Coenzyme Q10: Mitochondrial electron carrier [63]
- MitoQ: Mitochondria-targeted antioxidant [64]
- N-acetylcysteine: Glutathione precursor [65]
Free Radical Scavengers
- Edaravone: Approved for ALS [66]
- Tempol: SOD mimetic [67]
- Eukarion: Catalase mimetic [68]
Metabolic Support
- Creatine: Energy buffer [69]
- Alpha-lipoic acid: Mitochondrial cofactor [70]
- L-carnitine: Fatty acid transport [71]
Gene Therapy Approaches
- SOD1 overexpression: Mouse models show benefit [72]
- Nrf2 activation: Transcriptional upregulation of antioxidants [73]
Research Models
In Vitro
- H2O2 treatment: Acute oxidative stress [74]
- Glutamate excitotoxicity: Oxidative stress mechanism [75]
- Glucose oxidase: Continuous ROS generation [76]
- iPSC models: Patient-specific vulnerability [77]
In Vivo
- Paraquat administration: Parkinsonism model [78]
- Malonate injection: Complex II inhibition [79]
- 3-NP treatment: Huntington's disease model [80]
- Aging models: Natural oxidative damage accumulation [81]
See Also
- [Mitochondrially Impaired Neurons](/cell-types/mitochondrially-impaired-neurons)
- [Atrophic Neurons](/cell-types/atrophic-neurons)
- [Protein Aggregate-Bearing Neurons](/cell-types/protein-aggregate-bearing-neurons)
- [Alzheimer's Disease](/diseases/alzheimers-disease)
- [Parkinson's Disease](/diseases/parkinsons-disease)
- [Huntington's Disease](/diseases/huntington-disease)
- [Cell Types Index](/cell-types)
External Links
- [PubMed: Oxidative Stress in Neurodegeneration](https://pubmed.ncbi.nlm.nih.gov/) - Biomedical literature
- [Alzheimer's Association](https://www.alz.org/) - Research resources
- [Parkinson's Foundation](https://www.parkinson.org/) - Patient resources
- [ALS Association](https://www.als.org/) - Research and patient support
- [Allen Brain Atlas](https://brain-map.org/) - Gene expression data
Overview
Oxidatively Damaged Neurons plays an important role in the study of neurodegenerative diseases. This page provides comprehensive information about this topic, including its mechanisms, significance in disease processes, and therapeutic implications. [@kowluru2001]
Background
The study of Oxidatively Damaged Neurons has evolved significantly over the past decades. Research in this area has revealed important insights into the underlying mechanisms of neurodegeneration and continues to drive therapeutic development. [@bernardi1999]
Historical context and key discoveries in this field have shaped our current understanding and will continue to guide future research directions. [@detmer2007]
Additional evidence sources: [@sod2003] [@ruff1991] [@leonard2000] [@kelley1999] [@ron2007] [@berridge2002] [@klein2002] [@nixon2007] [@brunk2002] [@stoka2006] [@huang1999] [@hansson2008] [@bianca2009] [@jope2004] [@ebneth1998] [@hoyer2002] [@poon2005] [@zecca2004] [@butterfield2001] [@betarbet2000] [@valente2004] [@kitada1998] [@gerlach1994] [@stokes1999] [@fahn1992] [@block2005] [@sriram2006] [@gemma2007] [@cha2000] [@graveland1985] [@gunawardena2003] [@polidori1999] [@stoy2005] [@browne1999] [@sano1997] [@shults2002] [@murphy2007] [@sato2005] [@jubishi2017] [@wilcox2008] [@day2009] [@matthews1998] [@packer1997] [@sharma2009] [@gurney1994] [@kensler2007] [@ratan1994] [@coyle1993a] [@yang2002] [@kondo2013] [@mccormack2002] [@brouillet1999] [@brouillet2005] [@sohal1996]
Pathway Diagram
The following diagram shows the key molecular relationships involving Oxidatively Damaged Neurons discovered through SciDEX knowledge graph analysis:
▸Metadataorigin_type: v1_polymorphic_backfill
| slug | cell-types-oxidatively-damaged-neurons |
| kg_node_id | None |
| entity_type | cell |
| origin_type | v1_polymorphic_backfill |
| source_table | wiki_pages |
| wiki_page_id | wp-754a159a139e |
| __merged_from | {'merged_at': '2026-05-13', 'unprefixed_id': 'cell-types-oxidatively-damaged-neurons'} |
| _schema_version | 1 |
No provenance edges found
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