Blood Biomarker vs Tau PET for Treatment Monitoring

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experiment859 wordssynced 2026-04-02

Hypothesis

Primary Hypothesis: Blood-based biomarkers (p-tau217, p-tau181, NfL, GFAP) can serve as valid surrogates for tau PET in monitoring anti-tau therapeutic response, enabling more accessible and frequent monitoring in clinical trials and practice.

Secondary Hypotheses:

Blood p-tau217 changes correlate with tau PET changes (r > 0.7) over 12-24 month treatment periods

Blood biomarkers detect treatment effects earlier than tau PET due to higher sensitivity to change

The relationship between blood biomarkers and tau PET differs by therapeutic mechanism (antibody vs ASO vs small molecule)

Open Question Source

This experiment addresses the critical understanding gap identified in the [CBS/PSP Cure Roadmap](/mechanisms/cbs-psp-cure-roadmap) Phase 3:

"Can blood biomarkers substitute for tau PET in monitoring treatment response?"

Also addresses the practical constraint that tau PET is:

Expensive ($5,000-10,000/scan)
Limited availability (fewer than 50 US centers)
Involves radiation exposure
Not suitable for frequent monitoring

Validation Protocol

Study Design

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Hypothesis

Mermaid diagram (expand to render)

Secondary Hypotheses:

Blood p-tau217 changes correlate with tau PET changes (r > 0.7) over 12-24 month treatment periods

Blood biomarkers detect treatment effects earlier than tau PET due to higher sensitivity to change

The relationship between blood biomarkers and tau PET differs by therapeutic mechanism (antibody vs ASO vs small molecule)

Open Question Source

This experiment addresses the critical understanding gap identified in the [CBS/PSP Cure Roadmap](/mechanisms/cbs-psp-cure-roadmap) Phase 3:

"Can blood biomarkers substitute for tau PET in monitoring treatment response?"

Also addresses the practical constraint that tau PET is:

Expensive ($5,000-10,000/scan)
Limited availability (fewer than 50 US centers)
Involves radiation exposure
Not suitable for frequent monitoring

Validation Protocol

Study Design

Type: Prospective longitudinal biomarker correlation study embedded within Phase 2 anti-tau clinical trials
Cohort (pooled from multiple trials):
Anti-tau antibody trial participants (E2814, BMS-986446, Posdinemab): n=200
Tau ASO trial participants (BIIB080): n=100
OGA inhibitor trial participants (FNP-223): n=80
Total: n=380

Biomarker Collection Schedule

| Timepoint | Blood (p-tau217, NfL, GFAP) | CSF (p-tau181, total tau, NfL) | Tau PET |
|-----------|------------------------------|--------------------------------|---------|
| Baseline | ✓ | ✓ | ✓ |
| Month 1 | ✓ | ✓ | |
| Month 3 | ✓ | | |
| Month 6 | ✓ | ✓ | ✓ |
| Month 9 | ✓ | | |
| Month 12 | ✓ | ✓ | ✓ |
| Month 18 | ✓ | | ✓ |
| Month 24 | ✓ | ✓ | ✓ |

Clinical Assessments

Primary Endpoint: Correlation between blood p-tau217 % change and tau PET SUVr change at 12 months
Secondary Endpoints:
Correlation at other timepoints
Correlation with clinical measures (PSP-RS, CDR, MMSE)
Comparison across therapeutic mechanisms
Lead/lag analysis (which biomarker changes first)

Statistical Analysis Plan

Primary Analysis

Correlation analysis: Pearson and Spearman correlation between blood and PET biomarkers

Mixed-effects models: Account for repeated measures within subjects

Agreement analysis: Bland-Altman plots to assess agreement

Secondary Analyses

Sensitivity to change: Compare effect sizes (standardized mean differences) between biomarkers

Lead/lag analysis: Cross-correlation functions to identify temporal relationships

Subgroup analyses: By therapeutic mechanism, baseline disease severity, demographics

Surrogate Endpoint Validation Framework

Using the FDA BIOMARKER qualification framework:

Biological plausibility: Review evidence for causal relationship

Association: Correlation between surrogate and true endpoint

Predictive value: Ability to predict clinical outcome

Modulation by therapy: Evidence that therapy affects surrogate

Expected Outcomes

Primary Outcomes

Correlation coefficient: Blood p-tau217 vs tau PET at 12 months: r = 0.75 (95% CI: 0.65-0.82)

Sensitivity to change: Blood p-tau217 shows 1.5x larger effect size than tau PET

Minimum detectable effect: Blood biomarker can detect 20% treatment effect with n=100 per arm

Secondary Outcomes

Lead time: Blood biomarkers show significant change 3-6 months before tau PET

Mechanism-specific relationships: Different correlation patterns for antibody vs ASO vs OGAi

Clinical prediction: Blood biomarker changes at 6 months predict clinical outcome at 24 months

Exploratory Outcomes

Optimal biomarker panel: Identify combination of biomarkers that best predicts PET

Sampling frequency: Determine minimum sampling needed for adequate monitoring

Cost-effectiveness: Model cost savings from blood-based vs PET-based monitoring

Feasibility Assessment

Strengths

Leverages existing clinical trial infrastructure (reduces costs)
Multi-mechanism design enables mechanism-specific validation
Industry partnerships provide access to trial data
High clinical relevance for trial design

Challenges

Requires coordination across multiple pharma-sponsored trials
Different trial designs may limit direct comparisons
Blood biomarker assays lack standardization across labs
Tau PET acquisition protocols vary across sites

Timeline

| Milestone | Expected Date |
|-----------|---------------|
| Protocol development (with pharma partners) | Month 1-3 |
| Data sharing agreements | Month 3-6 |
| First patient data (pooled) | Month 6 |
| 50% enrollment | Month 12 |
| Full enrollment | Month 18 |
| 12-month primary analysis | Month 24 |
| 24-month analysis | Month 36 |
| FDA submission | Month 42 |

Cost Estimate

| Category | Cost (USD) |
|----------|------------|
| Personnel (1 FTE project manager, 1 biostatistician) | $600,000 |
| Blood biomarker assays (p-tau217, NfL, GFAP) | $400,000 |
| CSF biomarker assays | $200,000 |
| Tau PET (central reads) | $150,000 |
| Data management (harmonization across trials) | $300,000 |
| Statistical analysis | $200,000 |
| Regulatory consultation | $150,000 |
| Indirect costs (20%) | $400,000 |
| Total | $2,400,000 |

Note: Major cost share provided by pharma partners (trial sponsors)

Cross-Disease Relevance

This experiment has implications for:

AD (similar blood vs PET questions for amyloid)
Clinical trial design (enabling more frequent monitoring)
Clinical practice (accessibility for patients)
Biomarker qualification (FDA/EMA regulatory pathways)

Blood Biomarker vs Tau PET for Treatment Monitoring

Hypothesis

Open Question Source

Validation Protocol

Study Design

Hypothesis

Open Question Source

Validation Protocol

Study Design

Biomarker Collection Schedule

Clinical Assessments

Statistical Analysis Plan

Primary Analysis

Secondary Analyses

Surrogate Endpoint Validation Framework

Expected Outcomes

Primary Outcomes

Secondary Outcomes

Exploratory Outcomes

Feasibility Assessment

Strengths

Challenges

Timeline

Cost Estimate

Cross-Disease Relevance

See Also