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Blood Biomarker vs Tau PET for Treatment Monitoring

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experiment859 wordssynced 2026-04-02

Hypothesis

flowchart TD Cryptic_Hdgfl2["Cryptic Hdgfl2"] -->|"expressed in"| Blood["Blood"] HSPA1A["HSPA1A"] -->|"expressed in"| blood["blood"] HSPA1B["HSPA1B"] -->|"expressed in"| blood["blood"] style blood fill:#4fc3f7,stroke:#333,color:#000

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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