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SARM1 NADase Inhibition for Axonal Preservation

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idea2420 wordssynced 2026-04-02

SARM1 NADase Inhibition for Axonal Preservation

Overview

This therapeutic strategy targets SARM1 (Sterile Alpha and TIR Motif Containing 1), the genetically validated master executioner of Wallerian degeneration and programmed axon destruction. SARM1's intrinsic NADase activity rapidly depletes axonal NAD+ following injury or stress, triggering irreversible axon fragmentation. Pharmacological inhibition of SARM1's NADase domain represents one of the most compelling neuroprotective strategies across multiple neurodegenerative diseases where axonal degeneration is an early, driving pathology — including ALS, Parkinson's disease, and peripheral neuropathies.[@osterloh2012][@gerdts2013]

Target

  • Primary Target: SARM1 NADase catalytic domain (TIR domain)
  • Target Type: Small-molecule allosteric inhibitor or NAD+ competitive inhibitor
  • Expression: Exclusively neuronal; enriched in long-projection axons (motor neurons, nigrostriatal tract, peripheral sensory neurons)
  • Localization: Axonal mitochondria-associated; activated by rising NMN:NAD+ ratio upon mitochondrial stress

Mechanistic Rationale

Axonal degeneration precedes and often drives neuronal cell body death in most neurodegenerative diseases. The discovery that SARM1 is the obligate executioner of programmed axon degeneration — and that its genetic deletion provides complete axon protection — has made it one of the most validated neuroprotective targets in neuroscience.[@osterloh2012]

The SARM1 activation cascade:

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