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VCP Proteostasis Modulation Therapy for ALS/FTD

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idea1207 wordssynced 2026-04-02

Overview

VCP Proteostasis Modulation is a novel therapeutic strategy targeting the [Valosin Containing Protein (VCP](/proteins/vcp-p97)/p97), a genetically validated AAA+ ATPase that is mutated in amyotrophic lateral sclerosis (ALS), frontotemporal dementia (FTD), and inclusion body myopathy. VCP is essential for protein quality control, ER-associated degradation ([ERAD](/mechanisms/proteostasis-erad-pathway)), autophagosome maturation, and DNA repair — all pathways critically impaired in neurodegenerative disease.

Therapeutic Rationale

Genetic Evidence

[VCP](/proteins/vcp-p97) mutations cause a spectrum of neurodegenerative disorders[@johnson2010][@wong2020]:

  • IBMPFD (Inclusion Body Myopathy with Paget disease and Frontotemporal Dementia) — autosomal dominant
  • ALS — [VCP](/proteins/vcp-p97) mutations account for ~1-2% of familial ALS cases
  • FTD — [VCP](/proteins/vcp-p97) mutations found in familial FTD cases
  • PD — VCP variants associated with Parkinson's disease risk

The strong genetic evidence linking VCP to neurodegeneration makes it a compelling therapeutic target.

Mechanism

VCP functions as a molecular segregase that uses ATP hydrolysis to extract ubiquitinated substrates from membranes, protein complexes, and chromatin[@meyer2012][@watts2004]:

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