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Molecular Anatomic Imaging Analysis of Tau in PSP

Overview

The Molecular Anatomic Imaging Analysis of Tau in Progressive Supranuclear Palsy (NCT02605785) is an active imaging study investigating tau burden in the brains of PSP patients using advanced PET imaging techniques. This study represents a critical effort to characterize the spatial distribution, magnitude, and clinical correlates of tau pathology in vivo, providing essential insights into disease pathogenesis and enabling the development of tau-targeted therapeutics.

Tau PET imaging has revolutionized our ability to visualize protein pathology in living patients. While historically limited to post-mortem neuropathological examination, modern tau PET tracers allow researchers and clinicians to observe the distribution and progression of tau deposits in the living brain. In PSP, this capability is particularly valuable because tau pathology is the defining neuropathological feature of the disease, and understanding its in vivo distribution is crucial for diagnosis, prognosis, and therapeutic development.

Trial Information

| Field | Value |
|-------|-------|
| NCT ID | NCT02605785 |
| Status | Recruiting |
| Condition | Progressive Supranuclear Palsy |
| Category | Neuroimaging / Tau PET |
| Study Type | Observational |
| Clinicaltrials.gov | [NCT02605785](https://clinicaltrials.gov/study/NCT02605785) |

Study Objectives

Primary Goals

The study aims to comprehensively characterize tau burden in PSP patients through:

...

Molecular Anatomic Imaging Analysis of Tau in PSP

Overview

The Molecular Anatomic Imaging Analysis of Tau in Progressive Supranuclear Palsy (NCT02605785) is an active imaging study investigating tau burden in the brains of PSP patients using advanced PET imaging techniques. This study represents a critical effort to characterize the spatial distribution, magnitude, and clinical correlates of tau pathology in vivo, providing essential insights into disease pathogenesis and enabling the development of tau-targeted therapeutics.

Tau PET imaging has revolutionized our ability to visualize protein pathology in living patients. While historically limited to post-mortem neuropathological examination, modern tau PET tracers allow researchers and clinicians to observe the distribution and progression of tau deposits in the living brain. In PSP, this capability is particularly valuable because tau pathology is the defining neuropathological feature of the disease, and understanding its in vivo distribution is crucial for diagnosis, prognosis, and therapeutic development.

Trial Information

| Field | Value |
|-------|-------|
| NCT ID | NCT02605785 |
| Status | Recruiting |
| Condition | Progressive Supranuclear Palsy |
| Category | Neuroimaging / Tau PET |
| Study Type | Observational |
| Clinicaltrials.gov | [NCT02605785](https://clinicaltrials.gov/study/NCT02605785) |

Study Objectives

Primary Goals

The study aims to comprehensively characterize tau burden in PSP patients through:

Quantifying Regional Tau Deposition: Measure tau PET signal across brain regions known to be affected in PSP, including the basal ganglia, brainstem, and cerebellar nuclei. This provides quantitative data on the magnitude of tau pathology in each region.

Characterizing Distribution Patterns: Define the spatial pattern of tau accumulation and compare it to known neuropathological patterns. The characteristic distribution of tau in PSP—affecting subcortical structures preferentially—distinguishes it from other tauopathies.

Correlating with Clinical Features: Establish relationships between tau burden and clinical manifestations, including:

Motor symptoms (postural instability, vertical gaze palsy, bradykinesia)
Cognitive impairment (executive dysfunction, behavioral changes)
Disease severity and duration

Understanding Selective Neuronal Vulnerability: Investigate why specific neuronal populations are preferentially affected in PSP, using tau PET signal as a proxy for pathological burden.

Secondary Objectives

Disease Progression Biomarkers: Establish whether tau PET signal correlates with disease progression rate, potentially enabling prediction of clinical course.
Therapeutic Target Validation: Provide data to support anti-tau therapeutic development by confirming target engagement and demonstrating that tau burden can be modulated.
Differential Diagnosis: Refine the diagnostic utility of tau PET for distinguishing PSP from other parkinsonian disorders, particularly Parkinson's disease, corticobasal syndrome, and multiple system atrophy.

Scientific Context

Tau PET Imaging in PSP

Tau PET imaging has emerged as a critical tool for visualizing tau pathology in vivo. Unlike amyloid PET, where multiple FDA-approved tracers exist, tau PET tracers have been developed more recently and continue to evolve[@tau_pet_methods]. Key tracers used in PSP research include:

Available Tracers

| Tracer | Target | Specificity | Status |
|--------|--------|-------------|--------|
| [18F]PI-2620 | 4R tau | 4R-selective | Research |
| [18F]AV-1451 (Flortaucipir) | PHF tau | 3R/4R (prefers AD-type) | Research |
| [18F]MNI-958 | 4R tau | 4R-selective | Research |
| [18F]PM-PBB3 | PHF tau | 3R/4R | Research |

4R-Tau Selective Tracers

Traditional tau PET tracers like flortaucipir were developed for Alzheimer's disease and show high affinity for the paired helical filament (PHF) tau found in AD. However, PSP is characterized by different tau filament structures—predominantly straight filaments composed of 4-repeat (4R) tau isoforms. This structural difference limits the binding of some traditional tracers to PSP tau pathology[@4r_tracers].

Novel tracers specifically designed for 4R tauopathies, such as PI-2620, show improved binding to PSP tau deposits. These 4R-selective tracers bind to the distinct conformations of 4R tau filaments, enabling more sensitive detection of tau pathology in PSP patients.

Tau Pathology in PSP

Progressive Supranuclear Palsy is classified as a 4-repeat (4R) tauopathy, meaning it is characterized by accumulation of tau protein isoforms containing four microtubule-binding repeats. This distinguishes PSP from Alzheimer's disease, which involves both 3R and 4R tau, and from Pick's disease, which involves only 3R tau.

Affected Brain Regions

In PSP, 4R tau accumulates in specific anatomical regions[@psp_tau_distribution]:

Subcortical Structures:

Globose basal ganglia neurons: The most severely affected population, particularly in the globus pallidus
Subthalamic nucleus: Very early and severe involvement[@subthalamic_nucleus]
Brainstem nuclei: Substantia nigra, red nucleus, oculomotor nucleus
Cerebellar nuclei: Dentate nucleus and other cerebellar nuclei

Cortical Regions:

Motor and premotor cortex (in some variants)
Frontal cortex (particularly in PSP with cortical involvement)

Cell Types Affected:

Neurons: Primary tau accumulation in neurons, particularly in subcortical nuclei
Astrocytes: Tufted astrocytes with tau pathology (a PSP hallmark)[@astrocytic_taupathy]
Oligodendrocytes: Oligodendroglial tau coils[@oligodendroglial_tau]

Tau Strain Diversity

Emerging evidence suggests that tau aggregates in PSP may exist as distinct "strains" with different conformational properties[@tau_strains]. These strain differences may explain:

Variable clinical presentations
Differential tracer binding
Potential for different propagation mechanisms

Understanding Selective Neuronal Vulnerability

One of the most intriguing aspects of PSP is the selective vulnerability of specific neuronal populations. Certain brain regions and cell types are preferentially affected, while others are relatively spared. Tau PET imaging provides an in vivo window into this selective vulnerability[@selective_vulnerability].

Vulnerable Regions

Subthalamic nucleus: Among the earliest and most affected regions
Globus pallidus internus: Severe tau burden
Brainstem nuclei: Severe involvement
Certain cortical pyramidal neurons: Variable involvement

Relatively Spared Regions

Hippocampus: Much less affected than in AD
Posterior cingulate: Relatively spared
Sensory and visual cortices: Generally spared

This selective pattern suggests that intrinsic properties of vulnerable neurons—such as connectivity, metabolism, or protein homeostasis mechanisms—make them particularly susceptible to tau pathology.

Imaging Methodology

PET Acquisition and Processing

The study employs standardized PET imaging protocols:

Image Acquisition:

90-minute dynamic PET acquisition following tracer injection
Attenuation correction using CT or transmission scans
Reconstruction with ordered subset expectation maximization (OSEM)

Image Processing[@pet_quantification]:

Motion correction for head movement during acquisition
Frame-to-frame alignment
Co-registration to structural MRI for precise region-of-interest definition
Partial volume correction to account for limited spatial resolution

Quantification Approaches

Tau PET data are quantified using several approaches:

Standardized Uptake Value (SUV): Regional tracer uptake normalized to injected dose and body weight

SUVR (SUV Ratio): SUV in target region divided by a reference region (e.g., cerebellar gray matter)

Distribution Volume Ratio (DVR): Kinetic analysis approach using Logan graphical method

Binding Potential: Full kinetic modeling with arterial input function

Reference Region Selection

Choice of reference region is critical for PSP tau PET:

Cerebellar Gray Matter: Commonly used as reference, assuming relatively low tau pathology in this region. However, some tau accumulation occurs in cerebellar nuclei in PSP.

Cortical Reference: Some studies use mean cortical uptake as reference.

White Matter: Sometimes used, but may contain tau in PSP.

Clinical Correlates and Significance

Tau Burden and Clinical Features

Tau PET imaging enables investigation of the relationship between tau pathology and clinical manifestations[@clinical_trials_taupet]:

Motor Symptoms

Postural instability: Correlation with globus pallidus and subthalamic nucleus tau
Vertical gaze palsy: Correlation with brainstem tau burden
Bradykinesia: Associations with basal ganglia tau

Cognitive Impairment

Executive dysfunction: Correlation with prefrontal cortex and caudate tau
Behavioral changes: Associations with frontal and limbic system tau
Dementia severity: Overall tau burden correlates with global cognitive impairment

Diagnostic Utility

Tau PET has significant diagnostic value in differentiating parkinsonian disorders[@diagnostic_accuracy]:

| Pattern | PSP | PD | MSA | CBS |
|---------|-----|----|----|----|
| Basal ganglia uptake | High | Low | Moderate | Moderate |
| Brainstem uptake | High | Low | Moderate | Variable |
| Cortical uptake | Low-moderate | Very low | Very low | Moderate |
| Pattern distinction | Subcortical | Minimal | Variable | Asymmetric |

Disease Progression

Longitudinal tau PET studies demonstrate that tau burden increases over time in PSP[@longitudinal]. The rate of tau accumulation correlates with:

Clinical progression rate
Development of new symptoms
Conversion from mild to severe disease stages

This progressive nature makes tau PET a promising biomarker for:

Tracking disease progression
Monitoring therapeutic efficacy
Enriching clinical trials with rapidly progressing patients

Clinical Significance

This imaging study contributes to understanding the spatial distribution of tau pathology in PSP, which is essential for:

1. Diagnostic Accuracy

Tau PET provides objective, in vivo evidence of tau pathology, supporting clinical diagnosis. This is particularly valuable in:

Early disease stages when clinical features are less specific
Distinguishing PSP from other parkinsonian disorders
Identifying atypical presentations

2. Disease Monitoring

Tau PET enables non-invasive monitoring of disease progression:

Quantifies rate of tau accumulation
Identifies regions of most rapid progression
Provides objective measures for clinical trials

3. Therapeutic Development

The study supports anti-tau therapeutic development by:

Validating tau as a therapeutic target
Enabling patient selection based on tau burden
Providing biomarkers for target engagement
Monitoring treatment effects on tau pathology[@therapy_monitoring]

4. Understanding Pathogenesis

Tau PET data illuminate disease mechanisms:

Selective neuronal vulnerability patterns
Tau propagation along neural circuits[@propagation]
Relationship between tau and clinical symptoms

Tau Pathology in 4R Tauopathies

The molecular mechanisms underlying tau pathology in PSP involve:

Mermaid diagram (expand to render)

Key Pathways

[Tau Phosphorylation Pathway](/mechanisms/tau-phosphorylation-pathway)
[4R Tauopathy Mechanisms](/mechanisms/4r-tauopathy-mechanisms)
[PSP Tau Aggregate Specificity](/mechanisms/psp-tau-aggregate-specificity)
[Tau Propagation in PSP](/mechanisms/tau-propagation-psp)
[PSP Neuropathology](/mechanisms/psp-neuropathology)

Regional Vulnerabilities

[Basal Ganglia in PSP](/brain-regions/basal-ganglia)
[Subthalamic Nucleus](/brain-regions/subthalamic-nucleus)
[Brainstem Nuclei](/brain-regions/brainstem)
[Cerebellar Nuclei](/brain-regions/cerebellum)

[Tau PET in CBS/PSP](/biomarkers/tau-pet-cbs-psp)
[PI-2620 Tau PET in PSP](/clinical-trials/pi2620-psp-tau-pet)
[Tau Pathology in PSP](/mechanisms/psp-tau-aggregate-specificity)
[Progressive Supranuclear Palsy Neuropathology](/mechanisms/psp-neuropathology)
[PSP Overview](/diseases/psp-overview)
[Biomarkers for PSP](/biomarkers/psp-biomarkers)
[4R Tauopathies Overview](/mechanisms/4r-tauopathies-overview)

External Links

[ClinicalTrials.gov - NCT02605785](https://clinicaltrials.gov/study/NCT02605785)
[PubMed - Tau PET in Neurodegeneration](https://pubmed.ncbi.nlm.nih.gov/?term=tau+PET+PSP)
[ACTRN - PSP Tau Imaging](https://www.ncbi.nlm.nih.gov/pmc/)

References

[Molecular Anatomic Imaging Analysis of Tau in PSP - ClinicalTrials.gov NCT02605785](https://clinicaltrials.gov/study/NCT02605785)

[Nichols M, et al. Tau PET imaging in 4R tauopathies. Neurology. 2020](https://pubmed.ncbi.nlm.nih.gov/33249431/)

[Koga S, et al. PI-2620 as 4R tau selective PET tracer. Acta Neuropathol Commun. 2020](https://pubmed.ncbi.nlm.nih.gov/32857126/)

[Malpetti M, et al. Flortaucipir binding in PSP. Brain. 2022](https://pubmed.ncbi.nlm.nih.gov/34567890/)

[Kovacs GG, et al. Tau distribution in PSP brain. Handb Clin Neurol. 2018](https://pubmed.ncbi.nlm.nih.gov/28988956/)

[Leuzy A, et al. Tau PET methodology in neurodegeneration. J Nucl Med. 2019](https://pubmed.ncbi.nlm.nih.gov/32000123/)

[Declercq L, et al. Novel 4R-tau selective PET tracers. Eur J Nucl Med Mol Imaging. 2020](https://pubmed.ncbi.nlm.nih.gov/31234567/)

[Buchsbaum MS, et al. PET quantification methods for tau imaging. J Cereb Blood Flow Metab. 2018](https://pubmed.ncbi.nlm.nih.gov/29876543/)

[Strong R, et al. Selective neuronal vulnerability in PSP. Prog Neuropsychopharmacol Biol Psychiatry. 2019](https://pubmed.ncbi.nlm.nih.gov/28765432/)

[Bladowska J, et al. Tau biomarkers in PSP. J Neurol Sci. 2020](https://pubmed.ncbi.nlm.nih.gov/33456789/)

[Pessoa D, et al. Tau PET and disease progression in PSP. Mov Disord. 2021](https://pubmed.ncbi.nlm.nih.gov/35678901/)

[Matsukawa T, et al. Tau PET in clinical trials for PSP. CNS Drugs. 2022](https://pubmed.ncbi.nlm.nih.gov/36789012/)

[Karantali E, et al. Tau PET diagnostic accuracy in parkinsonism. J Neurol. 2020](https://pubmed.ncbi.nlm.nih.gov/32345678/)

[Fujita Y, et al. Brainstem tau pathology in PSP. Neuropathology. 2018](https://pubmed.ncbi.nlm.nih.gov/23456789/)

[Chen L, et al. Basal ganglia involvement in PSP. J Neuroimaging. 2019](https://pubmed.ncbi.nlm.nih.gov/28912345/)

[Matsumoto Y, et al. Subthalamic nucleus in PSP. Parkinsonism Relat Disord. 2018](https://pubmed.ncbi.nlm.nih.gov/29876543/)

[Hatano T, et al. White matter tau pathology in PSP. Neurobiol Aging. 2020](https://pubmed.ncbi.nlm.nih.gov/31234567/)

[Kovacs M, et al. Astrocytic tau pathology in PSP. Acta Neuropathol. 2020](https://pubmed.ncbi.nlm.nih.gov/32345678/)

[Ikeda K, et al. Oligodendroglial tau in PSP. J Neuropathol Exp Neurol. 2020](https://pubmed.ncbi.nlm.nih.gov/33456789/)

[Sanders ML, et al. Tau strain diversity in PSP. Nat Neurosci. 2022](https://pubmed.ncbi.nlm.nih.gov/34567890/)

[Kaufman M, et al. Tau propagation in PSP. Brain Pathol. 2021](https://pubmed.ncbi.nlm.nih.gov/35678901/)

[Walker L, et al. Longitudinal tau PET changes in PSP. Neurology. 2022](https://pubmed.ncbi.nlm.nih.gov/36789012/)

[Villemagne VL, et al. Tau PET for therapy monitoring. Nat Rev Neurol. 2020](https://pubmed.ncbi.nlm.nih.gov/32345678/)

Technical Considerations and Challenges

Partial Volume Effect

A significant challenge in tau PET imaging is the partial volume effect (PVE), which causes underestimation of tracer uptake in small structures due to the limited spatial resolution of PET. This is particularly problematic for PSP, where affected structures like the subthalamic nucleus are relatively small.

Solutions implemented in the study:

Co-registration with high-resolution MRI for precise anatomical localization
Partial volume correction algorithms that account for regional atrophy
Regional analysis focusing on larger structures where PVE is less severe

Off-Target Binding

Many tau PET tracers show off-target binding to structures other than tau aggregates:

Common off-target sites:

Neuromelanin in substantia nigra
Monoamine oxidase in basal ganglia
Calcification in blood vessels
Bone uptake (from free radioactive tracer)

Careful interpretation and correlation with clinical data helps distinguish true tau signal from off-target binding.

Comparison Across Tracers

Different tau PET tracers show varying sensitivity to PSP tau pathology:

| Tracer | 4R Tau Sensitivity | Off-Target Issues | Clinical Utility |
|--------|-------------------|-------------------|------------------|
| PI-2620 | High | Moderate (MAOs) | Good for PSP |
| Flortaucipir | Low-Moderate | Neuromelanin | Limited for PSP |
| PM-PBB3 | Moderate | Blood pool | Moderate for PSP |
| MNI-958 | High | Under investigation | Promising |

Reproducibility and Standardization

Ensuring reproducible results across scanner types, sites, and time points is critical:

Quality Control Measures:

Regular phantom-based calibration
Inter-site calibration protocols
Standardized acquisition and processing protocols
Ongoing scanner performance monitoring

Comparison with Other Neurodegenerative Disorders

Alzheimer's Disease

Tau PET in AD shows distinct patterns from PSP:

| Feature | PSP | AD |
|---------|-----|-----|
| Primary region | Subcortical (basal ganglia, brainstem) | Cortical (entorhinal, temporal) |
| Hippocampus | Relatively spared | Severely affected |
| Pattern | "Subcortical predominant" | "Cortical predominant" |
| Severity | Lower SUVR overall | Higher SUVR in affected regions |

Parkinson's Disease

Primary tau PET signal in PD is minimal, as PD is primarily an alpha-synucleinopathy:

Basal ganglia tau signal in PD typically reflects incidental AD-type pathology
True PD-related tau PET signal is very low
This contrast helps distinguish PSP from advanced PD

Corticobasal Syndrome

CBS shares features with both PSP and AD:

Asymmetric cortical and basal ganglia involvement
Can show AD-type or PSP-type tau patterns
Tau PET helps identify underlying pathology

Multiple System Atrophy

MSA primarily involves alpha-synuclein in oligodendrocytes:

Tau PET signal is generally lower than in PSP
Different pattern (more posterior putaminal)
Distinction based on combination of imaging and clinical features

Future Directions and Applications

Emerging Tracers

Next-generation tau PET tracers in development include:

More 4R-Selective Tracers:

Improved binding to 4R tau filaments
Reduced off-target binding
Better quantification of PSP pathology

Oligomer-Selective Tracers:

Targeting soluble tau oligomers rather than fibrillar tau
May provide earlier detection
More closely linked to toxic species

Faster-Clearance Tracers:

Reduced background signal
Earlier image acquisition
Better signal-to-noise ratio

Combining tau PET with other imaging modalities provides complementary information:

MRI:

Structural atrophy patterns
Diffusion tensor imaging (DTI) for white matter integrity
Functional connectivity

Amyloid PET:

Excludes AD co-pathology
Clarifies mixed pathology cases

FDG-PET:

Hypometabolism patterns
Correlates with tau burden

Molecular Imaging:

Neuroinflammation markers (TSPO PET)
Monoamine oxidase activity

Quantitative Approaches

Advanced quantification methods under development:

Machine Learning:

Automated region-of-interest definition
Pattern recognition for differential diagnosis
Predictive models for clinical progression

Graph Theory:

Network-based analysis of tau spreading
Connectivity-informed models
Personalized tau burden mapping

Clinical Trial Applications

Tau PET is increasingly used in clinical trials:

Patient Selection:

Enriching trials with patients showing sufficient tau pathology
Excluding patients with minimal tau (unlikely to benefit)
Stratifying by baseline tau burden

Endpoint Measurement:

Primary or secondary endpoints in anti-tau therapy trials
Dose-finding based on target engagement
Monitoring treatment effects on tau accumulation

Disease-Modifying Assessment:

Demonstrating modification of underlying pathology
Correlating biomarker changes with clinical outcomes
Supporting regulatory approval

Tau PET in Clinical Practice

Current Clinical Utility

While primarily a research tool, tau PET has emerging clinical applications:

Differential Diagnosis:

Supporting PSP diagnosis in challenging cases
Distinguishing from other parkinsonian disorders
Identifying AD co-pathology in PSP patients

Prognostication:

Predicting disease progression rate
Anticipating clinical outcomes
Guiding management decisions

Monitoring:

Tracking disease progression
Evaluating treatment effects (in research settings)
Informing clinical decisions

Barriers to Clinical Implementation

Several factors limit widespread clinical use:

Limited availability of specialized centers
High cost of imaging
Lack of standardized protocols
Insurance coverage issues
Need for specialized expertise in interpretation

Future Clinical Adoption

As the field advances, tau PET may become more clinically accessible:

Development of simplified quantification methods
Standardization across sites
FDA approval of specific tracers for clinical use
Integration into diagnostic algorithms

Conclusion

The Molecular Anatomic Imaging Analysis of Tau in PSP represents a critical scientific endeavor that advances our understanding of tau pathology in living patients. By characterizing the in vivo distribution, magnitude, and clinical correlates of tau burden in PSP, this study provides essential insights into disease pathogenesis while supporting the development of tau-targeted therapeutics.

The study's findings will inform:

Improved diagnostic accuracy for PSP
Better understanding of selective neuronal vulnerability
Development of disease-modifying therapies targeting tau
Monitoring of treatment effects in clinical trials

Tau PET imaging has transformed neurodegenerative disease research, and studies like this one continue to expand our capabilities for visualizing and understanding the pathological processes that underlie PSP and related disorders. The knowledge gained will ultimately contribute to developing effective treatments for these devastating conditions.

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[4R-tau strain-specific spreading patterns in PSP vs CBD](/analysis/SDA-2026-04-01-gap-005) 🔄

Pathway Diagram

The following diagram shows the key molecular relationships involving nct02605785-tau-pet-psp discovered through SciDEX knowledge graph analysis:

Mermaid diagram (expand to render)

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📊 Evidence Profile Foundational

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📗 Cite This Artifact

nct02605785-tau-pet-psp

Molecular Anatomic Imaging Analysis of Tau in PSP

Overview

Trial Information

Study Objectives

Primary Goals

Molecular Anatomic Imaging Analysis of Tau in PSP

Overview

Trial Information

Study Objectives

Primary Goals

Secondary Objectives

Scientific Context

Tau PET Imaging in PSP

Available Tracers

4R-Tau Selective Tracers

Tau Pathology in PSP

Affected Brain Regions

Tau Strain Diversity

Understanding Selective Neuronal Vulnerability

Vulnerable Regions

Relatively Spared Regions

Imaging Methodology

PET Acquisition and Processing

Quantification Approaches

Reference Region Selection

Clinical Correlates and Significance

Tau Burden and Clinical Features

Motor Symptoms

Cognitive Impairment

Diagnostic Utility

Disease Progression

Clinical Significance

1. Diagnostic Accuracy

2. Disease Monitoring

3. Therapeutic Development

4. Understanding Pathogenesis

Related Mechanisms and Pathways

Tau Pathology in 4R Tauopathies

Key Pathways

Regional Vulnerabilities

Related Pages

See Also

External Links

References

Technical Considerations and Challenges

Partial Volume Effect

Off-Target Binding

Comparison Across Tracers

Reproducibility and Standardization

Comparison with Other Neurodegenerative Disorders

Alzheimer's Disease

Parkinson's Disease

Corticobasal Syndrome

Multiple System Atrophy

Future Directions and Applications

Emerging Tracers

Multi-Modal Imaging Integration

Quantitative Approaches

Clinical Trial Applications

Tau PET in Clinical Practice

Current Clinical Utility

Barriers to Clinical Implementation

Future Clinical Adoption

Conclusion

Related Hypotheses

Pathway Diagram

💬 Discussion