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USP13 Inhibitor for Mitophagy and Synaptic Proteostasis

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USP13 Deubiquitinase Inhibition for Parkin-Independent Mitophagy Rescue

Overview

This therapeutic strategy targets USP13 (Ubiquitin-Specific Peptidase 13), a deubiquitinating enzyme that counteracts the ubiquitin-tagging of both Parkin and α-synuclein, thereby blocking their proteasomal degradation and impairing PINK1-Parkin mitophagy. Pharmacological inhibition of USP13 would restore ubiquitin-dependent clearance of damaged mitochondria and toxic α-synuclein species even in neurons with impaired Parkin function — a common feature of both familial and sporadic Parkinson's disease.[@liu2019][@liu2019a]

Target

  • Primary Target: USP13 (Ubiquitin-Specific Peptidase 13 / Isopeptidase T-3)
  • Target Type: Small-molecule catalytic-site inhibitor[@mevissen2017]
  • Expression: Broadly expressed; enriched in substantia nigra dopaminergic neurons and cortical neurons vulnerable in Lewy body dementia
  • Localization: Cytoplasm and outer mitochondrial membrane, where it opposes Parkin-mediated ubiquitination[@bingol2014]

Mechanistic Rationale

The PINK1-Parkin mitophagy pathway is the principal quality-control mechanism for damaged mitochondria in neurons.[@pickrell2015] When mitochondrial membrane potential collapses, PINK1 accumulates on the outer membrane and recruits Parkin, which ubiquitinates mitochondrial surface proteins to flag them for autophagic clearance.[@narendra2008] USP13 directly opposes this process at two levels:

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