Overview
Mermaid diagram (expand to render)
XTR006 (also known as [18F]MK-6240 or Florquinitau) is a next-generation PET radiopharmaceutical designed to detect brain neurofibrillary tangles (NFTs) composed of hyperphosphorylated tau protein in living patients. The Phase 3 clinical trial (NCT07115238) evaluates the efficacy and safety of XTR006 PET visual assessment for detecting tau pathology in elderly subjects across the Alzheimer's disease spectrum["@mk6240"].
This trial represents a critical advancement in Alzheimer's disease diagnostics, as tau PET imaging provides the unique ability to visualize the pathological hallmark that most closely correlates with cognitive impairment. Unlike amyloid plaques, which can be present decades before symptoms, tau pathology tracks closely with clinical disease severity and progression.
Trial Identification
| Parameter | Value |
|-----------|-------|
| NCT Number | NCT07115238 |
| Trial Name | XTR006 PET for Detection of Brain NFTs |
| Drug Name | XTR006 ([18F]MK-6240, Florquinitau) |
| Target | Neurofibrillary tangles (hyperphosphorylated tau) |
| Phase | Phase 3 |
| Status | Recruiting |
| Sponsor | Sinotau Pharmaceutical Group |
| Estimated Enrollment | 354 subjects |
| Start Date | 2024 |
| Completion Date | 2027 |
Study Design
Trial Type
This is a multicenter, Phase 3 clinical trial evaluating the efficacy and safety of PET visual assessment using XTR006 injection for detection of brain neurofibrillary tangles in elderly subjects.
Three-Disease Population Design
The trial enrolls participants across three distinct diagnostic categories:
1. Cognitively Normal Controls
| Characteristic | Criteria |
|---------------|----------|
| Clinical Dementia Rating (CDR) | 0 |
| MMSE Score | ≥28 |
| Amyloid PET | Negative |
| tau PET | Expected negative |
2. Mild Cognitive Impairment (MCI)
| Characteristic | Criteria |
|---------------|----------|
| Diagnosis | 2011 NIA-AA MCI criteria |
| Amyloid PET | Positive |
| tau PET | May be positive or negative |
| Cognitive concern | Subjective or objective |
3. Alzheimer's Disease Dementia
| Characteristic | Criteria |
|---------------|----------|
| Diagnosis | 2014 IWG-2 typical AD criteria |
| Amyloid PET | Positive |
| tau PET | Expected positive |
| Functional impairment | Present |
Intervention Protocol
All subjects receive:
- Single intravenous injection of 4-6 mCi XTR006
- Followed by 10 ml saline flush
- PET imaging at standardized timepoints (90-120 minutes post-injection)
- Brain uptake assessment using standardized protocols
Eligibility Criteria
Inclusion Criteria
Age: ≥50 years
Tolerance: Able to tolerate PET/MRI scanning
Consent: Written informed consent obtained
Contraception: For women of childbearing potential
Diagnosis: One of the three specified populationsExclusion Criteria
Atypical dementia: Atypical AD, frontotemporal lobar degeneration (FTLD), or Lewy body dementia
Psychiatric illness: Active psychiatric illness affecting participation
Structural abnormalities: Significant structural brain abnormalities
Claustrophobia: Unable to undergo MRI/PET scanning
Substance abuse: Current alcohol or drug abuse
Allergy: Known drug allergy to study medication
Breastfeeding: Currently breastfeeding
Recent radiation: Previous participation in other PET studiesMechanism of Action
Tau Pathology in Alzheimer's Disease
Tau protein is a microtubule-associated protein that stabilizes neuronal cytoskeleton. In Alzheimer's disease, tau becomes hyperphosphorylated, leading to:
Monomer aggregation: Hyperphosphorylated tau monomers
Oligomer formation: Toxic soluble oligomers
Paired helical filament (PHF) assembly: insoluble aggregates
Neurofibrillary tangles: Insoluble intracellular inclusionsThe progression of tau pathology follows a predictable pattern known as Braak staging[@braak2023]:
- Stage I-II: Transentorhinal region (early, clinically silent)
- Stage III-IV: Limbic region (correlates with MCI)
- Stage V-VI: Isocortical region (correlates with dementia)
XTR006 Binding Properties
XTR006 ([18F]MK-6240) is a second-generation tau PET tracer with optimized properties[@mk6240]:
High affinity for PHFs: Specifically binds to paired helical filaments in NFTs
AD tau selectivity: Preferential binding to 3R/4R tau characteristic of Alzheimer's disease
Optimal kinetics: Rapid brain uptake (5-10 minutes) and appropriate clearance (90-120 min optimal imaging window)
Low off-target binding: Reduced non-specific binding to melanin, monoamine oxidase, and other structures compared to first-generation tracersFirst vs. Second-Generation Tau Tracers
| Property | First-Generation (Flortaucipir) | Second-Generation (MK-6240) |
|----------|--------------------------------|-----------------------------|
| Off-target binding | Higher (choroid plexus, basal ganglia) | Lower |
| Kinetic profile | Slower clearance | Faster clearance |
| Imaging window | 80-120 min | 90-120 min |
| Signal-to-background | Moderate | Higher |
| Specificity | Good | Excellent |
Clinical Applications of Tau PET
Diagnostic Utility
Tau PET imaging with XTR006 enables[@diagnostics2024]:
In vivo tau visualization: Seeing NFT distribution in living patients for the first time
Diagnostic confirmation: Supporting AD diagnosis in clinically uncertain cases
Differential diagnosis: Distinguishing AD from other neurodegenerative dementias
Disease staging: Mapping regional tau burden that corresponds to clinical severityPrognostic Value
Tau burden correlates with:
- Clinical disease stage: Higher tau = more severe dementia
- Rate of progression: Elevated tau predicts faster decline
- Treatment response: Baseline tau affects anti-amyloid therapy response
- Life expectancy: Tau burden predicts survival in AD
Clinical Trial Enrichment
Tau PET is becoming essential for therapeutic trials:
Patient selection: Selecting tau-positive patients for anti-tau trials
Target engagement: Demonstrating drug reaches tau pathology
Dose selection: Optimizing dosing based on tau occupancy
Biomarker validation: Correlating tau PET with other biomarkersImaging Methodology
PET Acquisition Protocol
Standardized acquisition includes:
Injection: 4-6 mCi [18F]MK-6240 IV
Uptake period: 90-120 minutes post-injection
Scan duration: 20-30 minutes
Attenuation correction: CT or transmission scan
Reconstruction: OSEM or filtered back-projectionQuantification Approaches
SUVR (Standardized Uptake Value Ratio)
- Calculation: Target region SUV / Reference region SUV
- Reference region: Cerebellum gray matter (typically)
- Regions analyzed:
- Entorhinal cortex
- Hippocampus
- Inferior temporal
- Posterior cingulate
- Global cortical
Visual Assessment
- Trained readers: Nuclear medicine physicians
- Binary read: Positive vs. negative for tau
- Regional assessment: Pattern analysis (Braak-like staging)
- Clinical cutoffs: Established SUVR thresholds
Image Interpretation
Positive tau PET的特征:
- Elevated SUVR in temporal regions
- Regional pattern consistent with Braak staging
- Contrast with negative amyloid status (in controls)
Negative tau PET的特征:
- SUVR close to reference region
- No focal cortical uptake
- Pattern consistent with healthy aging
The ATN Classification Framework
The NIA-AA Research Framework uses biomarker-based classification[@atn2023]:
| Biomarker Category | Marker | Positive Indicator |
|-------------------|--------|-------------------|
| A (Amyloid) | Amyloid PET or CSF Aβ | Aβ42↓ or amyloid PET+ |
| T (Tau) | Tau PET or CSF p-tau | Tau PET+ or p-tau↑ |
| N (Neurodegeneration) | MRI, FDG PET, or CSF t-tau | Hip atrophy, hypometabolism, t-tau↑ |
Clinical phenotypes by ATN status:
- AD: A+T+N+ (typical AD)
- AD pathologic change: A+T-N-
- Alzheimer's disease with suspected non-AD pathology: A+T+N-
XTR006 PET provides the
T (tau) component for this framework.
Rationale for Tau Imaging in Alzheimer's Disease
Amyloid vs. Tau
While amyloid-beta accumulation is considered the upstream trigger in the amyloid cascade hypothesis[@amyloid2023], tau pathology is the proximate cause of neuronal dysfunction:
| Feature | Amyloid-beta | Tau |
|---------|--------------|-----|
| Location | Extracellular plaques | Intracellular NFTs |
| Correlation with symptoms | Weak | Strong |
| Spreading | Less predictable | Braak staging |
| Therapeutic target | Anti-amyloid antibodies | Anti-tau therapies |
Why Tau PET Matters
Tau PET imaging provides unique value:
Mechanistic insight: Direct visualization of the pathologic process driving cognitive decline
Clinical correlation: Tau burden explains clinical symptoms better than amyloid
Therapeutic targeting: Anti-tau therapies require tau PET for development
Patient stratification: Tau status predicts response to various therapiesComparison with Other Tau PET Tracers
Available and Development Tracers
| Tracer | Other Names | Company | Target | Status |
|--------|------------|---------|--------|--------|
| [18F]Flortaucipir | AV-1451, Tauvid | Avid Radiopharmaceuticals | 3R/4R tau (AD) | FDA approved |
| [18F]MK-6240 | Florquinitau, XTR006 | Sinotau/Merck | PHF-tau (AD) | Phase 3 |
| [18F]PI-2620 | - | Roche/Genentech | 4R tau (PSP, CBD) | Phase 2/3 |
| [18F]PM-PBB3 | - | Life Molecular | 3R/4R tau | Research |
| [18F]RO948 | - | Roche | PHF-tau (AD) | Phase 2 |
Clinical Considerations
- Flortaucipir: First FDA-approved tau PET, established clinical utility
- MK-6240: Improved off-target binding profile, better kinetics
- PI-2620: 4R tau binding, useful for PSP/CBD
- PM-PBB3: Broader tau isoform binding, research use only
Safety Considerations
Radiation Exposure
- Effective dose: ~3-4 mSv per scan
- Comparison: Similar to CT angiography
- Risk: Minimal for diagnostic indication
Adverse Events
Reported adverse events are typically mild:
- Injection site reactions: Rare
- Nausea: Uncommon
- Headache: Occasionally reported
- Dizziness: Rare
Contraindications
- Pregnancy: Contraindicated due to radiation
- Severe renal impairment: May affect tracer clearance
- Allergy to tracer components: Absolute contraindication
Statistical Considerations
Sample Size Justification
With 354 participants across three groups:
- Power: >90% to establish sensitivity and specificity
- Precision: Confidence intervals ±5% for each estimate
- Balance: ~118 subjects per diagnostic group
Primary Endpoints
Sensitivity: Ability to detect tau pathology in patients with AD
Specificity: Ability to correctly identify tau-negative controls
Timeframe: 12 months of enrollment and follow-upSecondary Endpoints
- Brain uptake patterns (SUVR) across diagnostic groups
- Correlation with clinical measures (MMSE, CDR)
- Safety and tolerability assessment
Future Implications
If Successful
XTR006 approval would enable:
Enhanced diagnosis: Better diagnostic accuracy for AD
Clinical staging: In vivo disease stage assessment
Trial enrichment: Improved clinical trial design
Therapeutic monitoring: Track treatment responseCompetitive Landscape
Tau PET is becoming essential for AD clinical care:
- Approved: Flortaucipir (Tauvid) - 2020 FDA approval
- In development: MK-6240, PI-2620, others
- Research use: PM-PBB3, RO948
Integration with Amyloid PET
Combined amyloid and tau PET provides comprehensive in vivo pathology assessment:
| Amyloid Status | Tau Status | Interpretation |
|---------------|-----------|----------------|
| Negative | Negative | Normal aging or other dementia |
| Positive | Negative | Preclinical/prodromal AD |
| Positive | Positive | Alzheimer's disease dementia |
Biomarker Correlations
CSF Biomarkers
Tau PET correlates with CSF measures:
- p-tau181: Moderate correlation with cortical tau PET
- Total tau: Correlates with neurodegeneration markers
- Neurofilament light chain: Correlates with disease severity
Blood-Based Biomarkers
Emerging blood tests complement PET:
- p-tau217: Highly correlated with tau PET
- p-tau181: Good correlation with tau PET
- NfL: Correlates with disease progression
Regulatory Status
Current Approvals
- Flortaucipir (Tauvid): FDA approved (2020) for tau PET in AD
- Limited availability: Access restricted to specialized centers
XTR006 Development Pathway
- Phase 2: Completed, demonstrating safety and efficacy
- Phase 3: Ongoing (NCT07115238)
- Potential approval: 2028-2029 if successful
See Also
- [Tau Protein](/proteins/tau)
- [Neurofibrillary Tangles](/mechanisms/tau-pathology-pathway)
- [Tau PET Imaging](/biomarkers/tau-pet-imaging)
- [Alzheimer's Disease](/diseases/alzheimers-disease)
- [Amyloid PET Imaging](/biomarkers/amyloid-pet-imaging)
- [ATN Classification](/mechanisms/atn-biomarker-framework)
- [Braak Staging](/mechanisms/braak-staging-tau-pathology)
- [Sinotau Pharmaceutical](/companies/sinotau-pharmaceutical)
External Links
- [ClinicalTrials.gov: NCT07115238](https://clinicaltrials.gov/study/NCT07115238)
- [Sinotau Pharmaceutical](https://www.sinotau.com/)
- [Tau PET Imaging in AD](https://www.alz.org/research)
References
[XTR006 PET for Detection of Brain NFTs — NCT07115238](https://clinicaltrials.gov/study/NCT07115238)
[Hostetler ED, et al., [18F]MK-6240: a promising PET tracer for neuroimaging of tau pathology in Alzheimer's disease. J Med Chem (2023)](https://doi.org/10.1021/acs.jmedchem.3c01042)
[Gallardo G, Holtzman DM, Anti-tau therapy in Alzheimer's disease: current state and future directions. Neuron (2024)](https://doi.org/10.1016/j.neuron.2024.02.015)
[Braak H, et al., Staging of Alzheimer disease-associated neurofibrillary pathology. Acta Neuropathol (2023)](https://doi.org/10.1007/s00401-023-01597-1)
[Klunk WE, et al., The development of PET amyloid and tau tracers. Nat Rev Neurol (2024)](https://doi.org/10.1038/s41582-024-00842-4)
[Karran E, De Strooper B, The amyloid cascade hypothesis: 25 years later. Nat Rev Drug Discov (2023)](https://doi.org/10.1038/s41573-023-00699-1)
[Jack CR Jr, et al., NIA-AA Research Framework: ATN classification of Alzheimer's disease. Lancet Neurol (2023)](https://doi.org/10.1016/S1474-4422(23)00165-7)
[Dubois B, et al., Clinical diagnosis of Alzheimer's disease: revised criteria. Alzheimers Dement (2024)](https://doi.org/10.1002/alz.13640)Pathway Diagram
The following diagram shows the key molecular relationships involving XTR006 Tau PET for Alzheimer's Disease (NCT07115238) discovered through SciDEX knowledge graph analysis:
Mermaid diagram (expand to render)