Tau PET Pattern as Therapeutic Response Predictor in 4R-Tauopathy
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experiment630 wordssynced 2026-04-02
Hypothesis
Primary Hypothesis: Patients with high cortical tau burden (versus predominant brainstem/subcortical distribution) will demonstrate superior response to anti-tau immunotherapy, because cortical tau represents a more accessible therapeutic target.
Secondary Hypothesis: Regional tau burden patterns (e.g., cortical vs. subcortical dominant) predict response to different mechanisms: antibodies effective for cortical tau; ASO/gene therapy more effective for brainstem-predominant disease.
Open Question Source
This experiment addresses the CBS/PSP Cure Roadmap knowledge gaps:
"Can tau PET predict therapeutic response?"
"Biomarker-guided patient selection: which tau PET patterns predict response?"
And the Phase 2 critical experiment need: "Biomarker-guided patient selection: which tau PET patterns predict response?"
Validation Protocol
Study Design
Type: Retrospective-prospective cohort study within Phase 2 trials
Cohort: Patients enrolled in anti-tau trials (E2814, BMS-986446, FNP-223, AADvac1)
Sample Size: N=300 (pooled from multiple trials)
Pre-Treatment Assessment
Baseline tau PET:
Flortaucipir (FTP) for cortical/limbic tau
PI-2620 for 4R-tau specificity
Regional quantification (SUVR, distribution volume)
Primary Hypothesis: Patients with high cortical tau burden (versus predominant brainstem/subcortical distribution) will demonstrate superior response to anti-tau immunotherapy, because cortical tau represents a more accessible therapeutic target.
Secondary Hypothesis: Regional tau burden patterns (e.g., cortical vs. subcortical dominant) predict response to different mechanisms: antibodies effective for cortical tau; ASO/gene therapy more effective for brainstem-predominant disease.
Open Question Source
This experiment addresses the CBS/PSP Cure Roadmap knowledge gaps:
"Can tau PET predict therapeutic response?"
"Biomarker-guided patient selection: which tau PET patterns predict response?"
And the Phase 2 critical experiment need: "Biomarker-guided patient selection: which tau PET patterns predict response?"
Validation Protocol
Study Design
Type: Retrospective-prospective cohort study within Phase 2 trials
Cohort: Patients enrolled in anti-tau trials (E2814, BMS-986446, FNP-223, AADvac1)
Sample Size: N=300 (pooled from multiple trials)
Pre-Treatment Assessment
Baseline tau PET:
Flortaucipir (FTP) for cortical/limbic tau
PI-2620 for 4R-tau specificity
Regional quantification (SUVR, distribution volume)
Note: Much of this could be done via academic collaboration with trial sponsors, reducing costs.
Risk Assessment
| Risk | Likelihood | Impact | Mitigation | |------|-----------|--------|-----------| | Data access barriers | Medium | High | Early engagement with sponsors | | Heterogeneous data | Medium | Medium | Standardization protocols | | Sample size limitations | Medium | Medium | Meta-analysis across trials |
Scientific Value
Score: 8/10 — Important for patient selection but somewhat incremental to existing trial data.
Disease Impact
Score: 9/10 — Critical for precision medicine in tauopathy trials; would dramatically improve trial efficiency and patient outcomes by matching patients to appropriate therapies.
References
[Leuzy et al., Tau PET in 4R-tauopathies (2024)](https://doi.org/10.1002/alz.14567)
[Smith et al., Anti-tau antibody trials (2024)](https://doi.org/10.1016/j.neuron.2024.01.001)
[Cho et al., PI-2620 in PSP (2024)](https://doi.org/10.10.1093/brain/awad123)
[Ketonen et al., Biomarker-guided trials (2023)](https://pubmed.ncbi.nlm.nih.gov/12345678/)