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ATP13A2/PARK9 Lysosomal Function Therapies for Parkinson's Disease

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ATP13A2/PARK9 Lysosomal Function Therapies for Parkinson's Disease

Overview

| Attribute | Value |
|-----------|-------|
| Category | Disease-Modifying Therapy |
| Target | ATP13A2/PARK9 lysosomal P5-ATPase |
| Diseases | Parkinson's Disease, Kufor-Rakeb Syndrome, Atypical Parkinsonism |
| Development Stage | Preclinical |
| Mechanism | Lysosomal calcium homeostasis, metal ion transport, autophagy regulation |

Introduction

[ATP13A2](/genes/atp13a2) (also known as [PARK9](/genes/atp13a2)) encodes a lysosomal P5-type ATPase that is critical for lysosomal function and neuronal survival. Loss-of-function mutations in [ATP13A2](/genes/atp13a2) cause Kufor-Rakeb syndrome (KRS), a rare autosomal recessive disorder characterized by [Parkinsonism](/diseases/parkinsons-disease), cognitive decline, and pyramidal tract involvement. [@ramirez2006]

Interestingly, common [ATP13A2](/genes/atp13a2) variants modify [Parkinson's disease](/diseases/parkinsons-disease) risk, and ATP13A2 expression is reduced in sporadic PD brains. This suggests that enhancing ATP13A2 function could have therapeutic benefit beyond rare genetic forms. [@chen2022]

ATP13A2 Biology

Protein Structure

ATP13A2 is a large transmembrane protein with:

  • P5-ATPase core: Catalytic domain for ion transport [@schultheis2004]
  • Lysosomal targeting sequence: Directs protein to lysosome [@kettner2021]
  • Multiple transmembrane domains: Spans lysosomal membrane [@sousa2019]

Normal Function


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mechanisms-atp13a2-park9-lysosomal-therapies-parkinsons
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