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Tau PROTAC and Degraders - Targeted Protein Degradation for Tau

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wiki page Created: 2026-04-02T07:19:56 By: crosslink-migration Quality: 50% ✓ SciDEX ID: wiki-mechanisms-tau-protac-deptac
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Tau PROTAC and Degraders: Targeted Protein Degradation for Tau

PROTACs (Proteolysis Targeting Chimeras) and other molecular degrader technologies represent a cutting-edge therapeutic strategy for treating tauopathies. These bifunctional molecules harness the cell's natural protein degradation machinery to selectively remove pathological tau protein.

Background: Targeted Protein Degradation

The PROTAC Mechanism


PROTACs are small molecules composed of two functional domains connected by a linker:
  • Tau-binding domain: Selectively binds to tau protein
  • E3 ligase recruiter: Binds to an E3 ubiquitin ligase complex
  • Linker: Connects the two domains
  • When a PROTAC brings a tau protein into proximity with an E3 ligase, the tau is ubiquitinated and targeted for degradation by the proteasome.

    Advantages Over Traditional Inhibition

    • Catalytic action: One PROTAC molecule can degrade multiple tau molecules
    • Undruggable targets: Can target proteins without defined active sites
    • Potential for disease modification: Complete removal of pathological protein
    • Oral bioavailability: Small molecules can be formulated as tablets

    Tau-Targeting PROTACs

    Development Challenges


    Developing tau PROTACs presents unique challenges:
  • Tau isoforms: Six tau isoforms require careful target selection
  • Intracellular location: Tau is primarily intracellular, requiring cell-permeable compounds
  • Aggregated tau: Insoluble aggregates may be less accessible
  • Brain penetration: Must cross the blood-brain barrier
  • ...
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