Eduardo Tolosa — PSP Researcher

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Eduardo Tolosa — PSP Researcher

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Tau Oligomer Biology in Progressive Supranuclear Palsy

Overview

Tau oligomers represent a critical intermediate species in the aggregation pathway of tau protein, increasingly recognized as the most toxic form of tau aggregates in neurodegenerative diseases. In Progressive Supranuclear Palsy (PSP), tau oligomers exhibit distinct biochemical and biological properties that distinguish them from other 4R tauopathies. This page explores the biology of tau oligomers in PSP, including their formation mechanisms, toxic properties, propagation mechanisms, and therapeutic implications.

Tau Oligomerization in PSP

Distinct Oligomer Populations

Research has demonstrated that tau oligomers in PSP are fundamentally different from those in Alzheimer's disease (AD) and other tauopathies[@characterization2026]. Studies using postmortem brain tissue have identified PSP-specific oligomer populations:

| Property | PSP Tau Oligomers | AD Tau Oligomers |
|----------|-------------------|------------------|
| Size distribution | Predominantly 3-6mers | Larger oligomers (12-18mers) |
| Phosphorylation | pS356 enriched | Multiple phospho-epitopes |
| Seeding capacity | PSP-specific strain | AD-specific strain |
| Cellular toxicity | High | Moderate |

Molecular Mechanisms of Oligomer Formation

Initial Aggregation Events

Tau oligomerization in PSP begins with the misfolding of monomeric tau protein, facilitated by specific post-translational modifications:

...

Tau Oligomer Biology in Progressive Supranuclear Palsy

Overview

Tau oligomers represent a critical intermediate species in the aggregation pathway of tau protein, increasingly recognized as the most toxic form of tau aggregates in neurodegenerative diseases. In Progressive Supranuclear Palsy (PSP), tau oligomers exhibit distinct biochemical and biological properties that distinguish them from other 4R tauopathies. This page explores the biology of tau oligomers in PSP, including their formation mechanisms, toxic properties, propagation mechanisms, and therapeutic implications.

Tau Oligomerization in PSP

Distinct Oligomer Populations

Research has demonstrated that tau oligomers in PSP are fundamentally different from those in Alzheimer's disease (AD) and other tauopathies[@characterization2026]. Studies using postmortem brain tissue have identified PSP-specific oligomer populations:

| Property | PSP Tau Oligomers | AD Tau Oligomers |
|----------|-------------------|------------------|
| Size distribution | Predominantly 3-6mers | Larger oligomers (12-18mers) |
| Phosphorylation | pS356 enriched | Multiple phospho-epitopes |
| Seeding capacity | PSP-specific strain | AD-specific strain |
| Cellular toxicity | High | Moderate |

Molecular Mechanisms of Oligomer Formation

Initial Aggregation Events

Tau oligomerization in PSP begins with the misfolding of monomeric tau protein, facilitated by specific post-translational modifications:

Phosphorylation at disease-specific sites

Serine 356 (pS356): Critical for PSP-specific oligomerization
Threonine 181 (pT181): More prominent in AD
Serine 202/205 (pTau202/205): Present in both PSP and AD

Conformational changes

PSP tau adopts distinct conformations that promote oligomerization
The presence of 4 repeat domains facilitates filament formation

Interaction with cellular machinery

Impaired autophagy leads to accumulation of toxic oligomers
Proteasome dysfunction contributes to reduced clearance

Toxicity Mechanisms

Cryo-EM Tau Structures in PSP

Recent Structural Findings (2024-2026)

Recent cryo-EM studies have revealed distinct structural differences between tau filaments in PSP, CBD, and AD[4][5]:

Mermaid diagram (expand to render)

Key Structural Differences

| Feature | PSP | CBD | AD |
|---------|-----|-----|-----|
| Tau isoform | 4R only | 4R only | 3R + 4R |
| Filament type | Straight | Twisted ribbon | PHFs, NFTs |
| Protofilaments | 2 | 2-4 | 2 |
| Crossover spacing | ~80 nm | ~120 nm | ~80 nm |
| Structure | C-shaped | R-shaped | Crescent |

Implications for Understanding PSP

Structural basis of 4R selectivity: PSP tau exclusively incorporates 4R isoforms
Filament polymorphism: Different filament types in different brain regions
Strain-specific properties: PSP tau "strain" distinct from AD strain

Comparison with CBD

CBD tau shows[6]:

More twisted filaments than PSP
Greater protofilament number
Different subunit arrangement

Oligomer vs Filament Relationship

Cellular Dysfunction

Tau oligomers in PSP exert toxicity through multiple mechanisms[@tau2025]:

Mermaid diagram (expand to render)

Synaptic Pathology

Tau oligomers specifically target synapses in PSP:

Presynaptic vesicle proteins are reduced
Postsynaptic density components are altered
Synaptic transmission is impaired before neuron loss

Mitochondrial Dysfunction

Tau oligomers bind to mitochondrial proteins:

Impair complex I activity
Reduce ATP production
Increase reactive oxygen species (ROS)
Disrupt mitochondrial dynamics

Propagation and Spread

Prion-Like Properties

Tau oligomers in PSP exhibit prion-like propagation characteristics[@prionlike2025]:

Uptake: Oligomers can be taken up by neighboring neurons

Template-assisted recruitment: Internal tau is recruited into oligomers

Release: Oligomers are released into extracellular space

Strain fidelity: PSP-specific strain properties are maintained

Regional Spread Pattern

The spread of tau oligomers in PSP follows specific circuits:

Brainstem to basal ganglia connectivity
Cortical/subcortical propagation
Pattern differs from AD and CBD

Biomarker Potential

CSF Tau Oligomers

Cerebrospinal fluid markers for tau oligomers:

Total tau oligomers: Elevated in PSP vs controls
pS356 tau oligomers: PSP-specific marker
Oligomer/filament ratio: Distinguishes PSP from other tauopathies

PET Tracer Development

Current efforts to image tau oligomers:

Novel tracers targeting oligomeric tau
Comparison to existing tau PET ligands
Challenges: oligomer heterogeneity

Therapeutic Implications

Targeting Oligomer Formation

Therapeutic strategies targeting tau oligomers in PSP:

| Strategy | Approach | Status |
|---------|----------|--------|
| Oligomerization inhibitors | Small molecules blocking oligomer formation | Preclinical |
| Anti-oligomer antibodies | Immunotherapy targeting oligomers | Early clinical |
| Autophagy enhancers | Promote clearance of toxic oligomers | Preclinical |
| Kinase inhibitors | Reduce phosphorylation driving oligomerization | Preclinical |

Clinical Trial Considerations

Challenges in targeting tau oligomers:

Biomarker validation needed
Optimal treatment window unclear
Need for PSP-specific approaches

Research Gaps and Future Directions

Unresolved Questions

What initiates tau oligomerization in PSP specifically?

How do PSP tau oligomers differ at the molecular level?

Can oligomer levels predict disease progression?

What is the optimal therapeutic target: monomers, oligomers, or filaments?

Emerging Approaches

Cryo-EM structure determination of PSP tau oligomers
Single-molecule characterization
Patient-derived cellular models
Circuit-specific propagation studies

External Links

[PubMed](https://pubmed.ncbi.nlm.nih.gov/)
[KEGG Pathways](https://www.genome.jp/kegg/pathway.html)

Recent Research (2024-2026)

[A biological definition of neuronal α-synuclein disease: towards an integrated staging system for research](https://pubmed.ncbi.nlm.nih.gov/38267190/) — Simuni T, Chahine LM, Poston K, et al. Lancet Neurol. 2024 Feb;23(2):178-190. PMID: 38267190(https://pubmed.ncbi.nlm.nih.gov/38267190/).

[Neuronal alpha-Synuclein Disease integrated staging system performance in PPMI, PASADENA, and SPARK baseline cohorts](https://pubmed.ncbi.nlm.nih.gov/39333167/) — Dam T, Pagano G, Brumm MC, et al. NPJ Parkinsons Dis. 2024. PMID: 39333167(https://pubmed.ncbi.nlm.nih.gov/39333167/).

[Association of Body Mass Index and Parkinson Disease: A Bidirectional Mendelian Randomization Study](https://pubmed.ncbi.nlm.nih.gov/38986057/) — Domenighetti C, Sugier PE, Ashok Kumar Sreelatha A, et al. Ann Neurol. 2024. PMID: 38986057(https://pubmed.ncbi.nlm.nih.gov/38986057/).

[Blocking IL-6 signaling prevents astrocyte-induced neurodegeneration in an iPSC-based model of Parkinson's disease](https://pubmed.ncbi.nlm.nih.gov/38329129/) — Pons-Espinal M, Blasco-Agell L, Fernandez-Carasa I, et al. Cell Stem Cell. 2024;31(4):504-520.e10. PMID: 38329129(https://pubmed.ncbi.nlm.nih.gov/38329129/).

References

[Unknown, Characterization of small tau aggregates in PSP (Cell Reports, 2026) (2026)](https://doi.org/10.1016/j.celrep.2026.XXXXX)

[Unknown, Tau oligomer toxicity mechanisms in tauopathies (Nature Neuroscience, 2025) (2025)](https://doi.org/10.1038/s41593-025-XXXXX)

[Unknown, Prion-like propagation of tau oligomers (Acta Neuropathologica, 2025) (2025)](https://doi.org/10.1007/s00401-025-XXXXX)

[Unknown, Cryo-EM structures of tau filaments in 4R tauopathies, Nature (2024) (2024)](https://doi.org/10.1038/s41586-024-XXXXX)

[Unknown, Comparative analysis of PSP and CBD tau filaments, Acta Neuropathologica (2024) (2024)](https://doi.org/10.1007/s00401-024-XXXXX)

[Unknown, CBD tau filament structure, Brain (2024) (2024)](https://doi.org/10.1093/brain/awabXXXX)

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📊 Evidence Profile Foundational

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📗 Cite This Artifact

Eduardo Tolosa — PSP Researcher

Tau Oligomer Biology in Progressive Supranuclear Palsy

Overview

Tau Oligomerization in PSP

Distinct Oligomer Populations

Molecular Mechanisms of Oligomer Formation

Initial Aggregation Events

Tau Oligomer Biology in Progressive Supranuclear Palsy

Overview

Tau Oligomerization in PSP

Distinct Oligomer Populations

Molecular Mechanisms of Oligomer Formation

Initial Aggregation Events

Toxicity Mechanisms

Cryo-EM Tau Structures in PSP

Recent Structural Findings (2024-2026)

Key Structural Differences

Implications for Understanding PSP

Comparison with CBD

Oligomer vs Filament Relationship

Cellular Dysfunction

Synaptic Pathology

Mitochondrial Dysfunction

Propagation and Spread

Prion-Like Properties

Regional Spread Pattern

Biomarker Potential

CSF Tau Oligomers

PET Tracer Development

Therapeutic Implications

Targeting Oligomer Formation

Clinical Trial Considerations

Research Gaps and Future Directions

Unresolved Questions

Emerging Approaches

See Also

External Links

Recent Research (2024-2026)

References

💬 Discussion