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TDP-43 Proteinopathy in ALS
TDP-43 Proteinopathy in ALS
Introduction
Tdp 43 Proteinopathy In Als represents a key pathological mechanism in neurodegenerative diseases. This page explores the molecular and cellular processes involved, their contribution to disease progression, and therapeutic implications.
Overview
TDP-43 (TAR DNA-binding protein 43) is a nuclear RNA/DNA-binding protein that is central to the pathogenesis of most cases of Amyotrophic Lateral Sclerosis (ALS) and Frontotemporal Dementia (FTD). Pathological TDP-43 aggregation is found in approximately 95% of ALS cases and 50% of FTD cases, making it a key therapeutic target. [@arai2006]
Pathway Diagram
Molecular Mechanisms
1. TDP-43 Normal Function
TDP-43 is a heterogeneous nuclear ribonucleoprotein (hnRNP) with essential functions: [@sreedharan2008]
- DNA binding: Binds to TAR DNA sequences (TG-rich)
- RNA splicing: Regulates alternative splicing of thousands of transcripts
- RNA stability: Controls mRNA turnover and transport
- Stress response: Forms stress granules under cellular stress
2. Pathological Mislocalization
In disease, TDP-43 undergoes characteristic changes: [@johnson2009]
TDP-43 Proteinopathy in ALS
Introduction
Tdp 43 Proteinopathy In Als represents a key pathological mechanism in neurodegenerative diseases. This page explores the molecular and cellular processes involved, their contribution to disease progression, and therapeutic implications.
Overview
TDP-43 (TAR DNA-binding protein 43) is a nuclear RNA/DNA-binding protein that is central to the pathogenesis of most cases of Amyotrophic Lateral Sclerosis (ALS) and Frontotemporal Dementia (FTD). Pathological TDP-43 aggregation is found in approximately 95% of ALS cases and 50% of FTD cases, making it a key therapeutic target. [@arai2006]
Pathway Diagram
Molecular Mechanisms
1. TDP-43 Normal Function
TDP-43 is a heterogeneous nuclear ribonucleoprotein (hnRNP) with essential functions: [@sreedharan2008]
- DNA binding: Binds to TAR DNA sequences (TG-rich)
- RNA splicing: Regulates alternative splicing of thousands of transcripts
- RNA stability: Controls mRNA turnover and transport
- Stress response: Forms stress granules under cellular stress
2. Pathological Mislocalization
In disease, TDP-43 undergoes characteristic changes: [@johnson2009]
- Nuclear depletion: Loss of nuclear TDP-43
- Cytoplasmic aggregation: Formation of stress granules and inclusions
- Phosphorylation: Hyperphosphorylation at Ser409/410
- Ubiquitination: Post-translational modification
- C-terminal fragmentation: Generation of toxic fragments
3. Loss of Nuclear Function
Nuclear TDP-43 loss disrupts: [@buratti2005]
Splicing dysregulation: [@sephton2011]
- Cryptic exon inclusion
- Exon skipping
- Inappropriate splicing of:
- Neuronal development genes
- Synaptic function genes
- Mitochondrial function genes
- Impaired mRNA transport
- Reduced translation
- Altered RNA stability
4. Gain of Cytoplasmic Toxicity
Cytoplasmic TDP-43 aggregates cause: [@liu2017]
Stress granule dysfunction: [@rascovsky2011]
- Sequestration of translation machinery
- Impaired stress response
- Persistence of stress granules
- Direct binding to mitochondria
- Impaired mitochondrial trafficking
- Reduced ATP production
- Nuclear export dysregulation
- Nucleocytoplasmic transport defects
Genetic Causes
ALS-Causing Mutations
| Gene | Mutation Effect | % of ALS | [@prasad2019]
|------|---------------|----------| [@hunter2021]
| TARDBP | Autosomal dominant | ~3-5% | [@frontini2022]
| FUS | Autosomal dominant | ~3-5% |
| C9orf72 | Hexanucleotide repeat | ~40% |
| TIA1 | Stress granule regulation | ~1% |
Mutations Affecting TDP-43
- TARDBP: Direct mutations in TDP-43 coding region
- FUS: FUS protein sequesters TDP-43
- C9orf72: RNA foci sequester TDP-43
- TIA1: Stress granule dynamics altered
- OPTN: Autophagy impairment affects clearance
Disease Associations
Amyotrophic Lateral Sclerosis (ALS)
- 95% of ALS cases have TDP-43 pathology
- All sporadic ALS cases
- All non-SOD1 familial ALS
- Includes C9orf72, FUS, TARDBP mutations
Frontotemporal Dementia (FTD)
- 50% of FTD cases have TDP-43 pathology
- FTLD-TDP subtype
- Behavioral variant FTD (bvFTD)
- Primary progressive aphasia (PPA)
ALS-FTD Spectrum
- Overlapping clinical features
- Shared pathology (TDP-43)
- Common genetic causes (C9orf72)
- ~15% of patients develop both
Therapeutic Implications
Strategies Under Development
- Small molecules targeting protein-protein interactions
- Compounds promoting clearance
- Antisense oligonucleotides for TARDBP mutations
- Splicing modulators
- Inhibitors of stress granule formation
- Compounds promoting dissolution
- Antioxidants
- Mitochondrial biogenesis inducers
- TFEB activators
- Autophagy-inducing compounds
Biomarkers
- CSF TDP-43: Diagnostic potential
- Phospho-TDP-43: Disease-specific
- Neurofilaments: Disease progression
- PET tracers: In development
Cross-Links
- ALS Overview
- C9orf72 ALS Pathway
- SOD1 ALS Pathway
- FTD-TDP43 Pathway
- [Stress Granules](/mechanisms/stress-granules)
- [Mitochondrial Dysfunction](/mechanisms/mitochondrial-dysfunction)
Background
The study of Tdp 43 Proteinopathy In Als 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.
Historical context and key discoveries in this field have shaped our current understanding and will continue to guide future research directions.
See Also
- [Alzheimer's Disease](/diseases/alzheimers-disease)
- [Amyloid Hypothesis](/mechanisms/amyloid-hypothesis)
- [Tau Pathology](/mechanisms/tau-pathology)
- [Parkinson's Disease](/diseases/parkinsons-disease)
- [Alpha-Synuclein Pathway](/mechanisms/alpha-synuclein-pathology)
External Links
- [PubMed](https://pubmed.ncbi.nlm.nih.gov/) - Biomedical literature
- [Alzheimer's Disease Neuroimaging Initiative](https://adni.loni.usc.edu/) - Research data
- [Allen Brain Atlas](https://brain-map.org/) - Brain gene expression data
Confidence Assessment
🟡 Moderate Confidence
| Dimension | Score |
|-----------|-------|
| Supporting Studies | 15 references |
| Replication | 0% |
| Effect Sizes | 25% |
| Contradicting Evidence | 0% |
| Mechanistic Completeness | 75% |
Overall Confidence: 45%
Recent Research Updates (2024-2026)
- [Hruska-Plochan M et al., Nature (2024 Feb)](https://pubmed.ncbi.nlm.nih.gov/38355792/)
- [Eisen A et al., Prog Neurobiol (2024 Mar)](https://pubmed.ncbi.nlm.nih.gov/38266701/)
- [Keeley O et al., Acta Neuropathol Commun (2024 Dec 21)](https://pubmed.ncbi.nlm.nih.gov/39709457/)
- [Zamani A et al., Neurobiol Dis (2025 Mar)](https://pubmed.ncbi.nlm.nih.gov/39914774/)
- [Dubey SK et al., Neuron (2026 Mar 4)](https://pubmed.ncbi.nlm.nih.gov/41475349/)
Additional Reading
TDP-43 Aggregation Mechanisms
Structural Basis of Aggregation
TDP-43 contains multiple domains that contribute to its aggregation propensity:
- N-terminal domain (1-414): Contains the nuclear localization signal (NLS) and the RNA recognition motif (RRM1)
- RRM1 (104-262): Binds to UG-rich RNA sequences
- RRM2 (262-350): Additional RNA-binding capacity
- Low-complexity domain (LCD, 341-414): Intrinsically disordered region critical for phase separation and aggregation
Post-Translational Modifications
Pathological TDP-43 is characterized by specific PTMs:
| Modification | Site | Significance |
|--------------|------|--------------|
| Phosphorylation | Ser409/Ser410 | Disease-specific, drives aggregation |
| Phosphorylation | Ser379/Ser403/Ser409 | Multiple sites in patient tissue |
| Ubiquitination | Lys residues | Marks for proteasomal degradation |
| Sumoylation | Lys residues | May promote aggregation |
| C-terminal truncation | Various sites | Generates toxic fragments |
Aggregation Kinetics
- Primary nucleation: Spontaneous assembly of TDP-43 monomers
- Secondary nucleation: Seeding by existing aggregates
- Surface-catalyzed nucleation: Growth on foreign surfaces
- Oligomer formation: Toxic intermediate species
- Fibril elongation: Formation of inclusions
TDP-43 in RNA Metabolism
Essential RNA Targets
TDP-43 regulates splicing and stability of critical neuronal transcripts:
| Function | Key Targets | Disease Relevance |
|----------|-------------|-------------------|
| Neuronal development | UNC13A, STX3, PRKN | Developmental defects |
| Synaptic function | SYN1, DLGL1, CACNA2D3 | Synaptic dysfunction |
| Mitochondrial function | NDUFA2, ATP5F1B | Energy deficits |
| Axonal transport | DYNC1H1, KIF5C | Axonal pathology |
| RNA splicing | Cryptic exons in multiple genes | Global splicing disruption |
Cryptic Exon Inclusion
One of the most significant consequences of TDP-43 loss:
- UNC13A cryptic exons: Inclusion creates truncated non-functional protein
- Other targets: SEMA3B, SEL1L, RIMBP2
- Functional consequences: Loss of essential neuronal proteins
- Therapeutic opportunity: Antisense oligonucleotides can block cryptic exons
TDP-43 in Other Neurodegenerative Diseases
Alzheimer's Disease
- TDP-43 pathology found in ~20-30% of AD cases
- Often coexists with tau and amyloid pathology
- Associated with greater cognitive impairment
- May represent a distinct disease subtype
Parkinson's Disease
- TDP-43 in ~10-15% of PD cases
- Associated with rapid disease progression
- More common in certain genetic forms (LRRK2, GBA)
Limbic-Predominant Age-Related TDP-43 Encephalopathy (LATE)
- TDP-43 pathology in aging brain
- Clinically resembles Alzheimer's disease
- Affects limbic structures preferentially
- High prevalence in individuals over 80
Experimental Models
In Vitro Models
- Purified protein aggregation: Recombinant TDP-43 LCD forms fibrils
- Cell lines: Transient transfection of mutant TDP-43
- iPSC-derived neurons: Patient-derived motor neurons
- Organoids: Brain organoids with TDP-43 pathology
In Vivo Models
- TARDBP transgenic mice: Wild-type and mutant TDP-43
- Conditional models: Inducible TDP-43 expression
- Knock-in models: Endogenous TDP-43 mutations
- Viral-mediated expression: AAV-delivered TDP-43
Therapeutic Strategies
RNA-Targeted Approaches
| Approach | Mechanism | Stage |
|----------|-----------|-------|
| ASOs for TARDBP | Reduce mutant TDP-43 | Preclinical |
| Splicing modulators | Prevent cryptic exon inclusion | Preclinical |
| RNA stabilizers | Enhance nuclear TDP-43 function | Preclinical |
Protein-Targeted Approaches
| Approach | Mechanism | Stage |
|----------|-----------|-------|
| Aggregation inhibitors | Block protein-protein interactions | Preclinical |
| Small molecule stabilizers | Prevent misfolding | Preclinical |
| Antibody therapies | Anti-TDP-43 antibodies | Preclinical |
Enhancing Clearance
| Approach | Mechanism | Stage |
|----------|-----------|-------|
| Autophagy enhancers | TFEB activators | Preclinical |
| Proteasome enhancers | Increase degradation | Preclinical |
| Immunotherapies | Antibody-mediated clearance | Preclinical |
Biomarker Development
Diagnostic Biomarkers
- Phospho-TDP-43 in CSF: Highly specific for TDP-43 proteinopathy
- Total TDP-43 in CSF: Elevated in disease
- NfL in blood/CSF: General neurodegeneration marker
Prognostic Biomarkers
- Disease progression: Rate of NfL change
- Therapeutic response: Changes in TDP-43 species
- Phenotype prediction: TDP-43 pathology pattern
Monitoring Biomarkers
- PET tracers: In development for TDP-43
- Peripheral markers: Blood cells, skin fibroblasts
- Neuroimaging: TDP-43-related structural changes
References
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Pathway Diagram
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SciDEX Links
Related Hypotheses
- [Bacterial Enzyme-Mediated Dopamine Precursor Synthesis](/hypothesis/h-7bb47d7a) — score 0.59; target TH, AADC; neurodegeneration.
- [Cryptic Exon Silencing Restoration](/hypothesis/h-4fabd9ce) — score 0.53; target TARDBP; neurodegeneration.
- [Cross-Seeding Prevention Strategy](/hypothesis/h-eea667a9) — score 0.69; target TARDBP; neurodegeneration.
- [Glycine-Rich Domain Competitive Inhibition](/hypothesis/h-7e846ceb) — score 0.64; target TARDBP; neurodegeneration.
Related Analyses
- [TDP-43 phase separation therapeutics for ALS-FTD](/analyses/sda-2026-04-01-gap-006)
- [What determines the selectivity and efficiency of intercellular transmission pathways for different misfolded proteins?](/analyses/SDA-2026-04-08-gap-pubmed-20260406-062207-5a703c17)
- [What is the therapeutic window between insufficient and toxic levels of TDP-43 arginine methylation?](/analyses/SDA-2026-04-12-gap-debate-20260410-113051-5dce7651)
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