KIAA0196 (WASHC5) Gene

KIAA0196 (WASHC5) Gene

Introduction

The KIAA0196 gene (now officially known as WASHC5, WASH Complex Subunit 5, also called Strumpellin) encodes a core component of the WASH complex that regulates endosomal protein sorting and recycling. Mutations cause autosomal dominant hereditary spastic paraplegia type 8 (SPG8).

Overview

The KIAA0196/WASHC5 gene is located on chromosome 8q24.13 and encodes strumpellin, a 1,159-amino acid protein that forms part of the WASH (Wiskott-Aldrich syndrome protein and SCAR homolog) complex^[1]. The WASH complex regulates actin polymerization on endosomes, which is essential for the tubular recycling of membrane proteins including receptors and transporters^[2]. Heterozygous missense mutations cause SPG8, a pure form of autosomal dominant hereditary spastic paraplegia (HSP) characterized by progressive spasticity of the lower limbs due to corticospinal tract degeneration^[3]. [@derivery2009]

<div class="infobox infobox-gene"> [@de2013]

KIAA0196 (WASHC5) Gene

Introduction

The KIAA0196 gene (now officially known as WASHC5, WASH Complex Subunit 5, also called Strumpellin) encodes a core component of the WASH complex that regulates endosomal protein sorting and recycling. Mutations cause autosomal dominant hereditary spastic paraplegia type 8 (SPG8).

Overview

The KIAA0196/WASHC5 gene is located on chromosome 8q24.13 and encodes strumpellin, a 1,159-amino acid protein that forms part of the WASH (Wiskott-Aldrich syndrome protein and SCAR homolog) complex^[1]. The WASH complex regulates actin polymerization on endosomes, which is essential for the tubular recycling of membrane proteins including receptors and transporters^[2]. Heterozygous missense mutations cause SPG8, a pure form of autosomal dominant hereditary spastic paraplegia (HSP) characterized by progressive spasticity of the lower limbs due to corticospinal tract degeneration^[3]. [@derivery2009]

<div class="infobox infobox-gene"> [@de2013]

| | | [@freeman2015]
|---|---| [@mcgough2014]
| Gene Symbol | WASHC5 (formerly KIAA0196) |
| Full Name | WASH Complex Subunit 5 (Strumpellin) |
| Aliases | KIAA0196, SPG8, Strumpellin |
| Chromosomal Location | 8q24.13 |
| NCBI Gene ID | [9744](https://www.ncbi.nlm.nih.gov/gene/9744) |
| OMIM | [610657](https://omim.org/entry/610657) |
| Ensembl | [ENSG00000104523](https://www.ensembl.org/Homo_sapiens/Gene/Summary?g=ENSG00000104523) |
| UniProt | [Q12768](https://www.uniprot.org/uniprot/Q12768) |
| Associated Diseases | SPG8 (hereditary spastic paraplegia type 8) |

</div>

Function

WASH Complex

Strumpellin is one of five core subunits of the WASH complex^[2]:

| Subunit | Gene | Function |
|---------|------|----------|
| WASH1 | WASHC1 | Arp2/3 activator; nucleates actin on endosomes |
| FAM21 | WASHC2 | Connects WASH complex to retromer via VPS35 |
| CCDC53 | WASHC3 | Structural subunit |
| SWIP | WASHC4 | Structural subunit |
| Strumpellin | WASHC5 (KIAA0196) | Structural/regulatory subunit; connects to VAMP-associated proteins |

The WASH complex nucleates branched actin filaments on endosomal membranes, creating force for membrane tubulation and cargo sorting^[2].

Endosomal Protein Recycling

Strumpellin is essential for proper endosomal recycling^[4]:

• Cargo sorting: Enables recycling of cell surface receptors (transferrin receptor, integrins, glucose transporters) from endosomes back to the plasma membrane
• Retromer cooperation: WASH complex works with the retromer ([VPS35](/genes/vps35)) to sort cargo from endosome-to-Golgi and endosome-to-surface pathways
• Membrane remodeling: Actin-driven tubulation creates recycling tubules from endosomal compartments
• Receptor trafficking: Required for proper trafficking of signaling receptors in [neurons](/entities/neurons)

Neuronal Significance

In neurons, endosomal recycling is critical for^[3]:

• Axonal transport: Long corticospinal axons require efficient endosomal trafficking
• Synaptic receptor recycling: AMPA and [NMDA receptor](/entities/nmda-receptor) surface expression depends on endosomal sorting
• Neurotrophic factor signaling: [BDNF](/genes/bdnf)/TrkB retrograde signaling endosomes
• [Autophagy](/entities/autophagy): Endosomal maturation feeds into the autophagic pathway

Disease Associations

Hereditary Spastic Paraplegia Type 8 (SPG8)

SPG8 is a pure autosomal dominant HSP caused by WASHC5 mutations^[3]:

| Feature | Description |
|---------|-------------|
| Inheritance | Autosomal dominant |
| Onset | Variable (childhood to 5th decade, mean ~30-40 years) |
| Core feature | Progressive spastic paraparesis (lower limb spasticity) |
| Gait | Scissoring gait, hyperreflexia, extensor plantar responses |
| Upper limbs | Usually spared (pure HSP) |
| Bladder | Urinary urgency common |
| Cognition | Usually preserved |
| Neuropathology | Corticospinal tract (axonal) degeneration, length-dependent |

Pathogenic Mechanism

SPG8-causing mutations impair strumpellin function through^[4]:

• Endosomal recycling defects: Impaired cargo sorting leads to receptor mislocalization
• Axonal degeneration: The longest axons (corticospinal, >1 meter) are most vulnerable to endosomal trafficking defects
• Length-dependent vulnerability: Distal axonal regions farthest from the cell body degenerate first
• Retromer dysfunction: Impaired WASH-retromer cooperation reduces VPS35-mediated sorting

Connections to Other Neurodegenerative Diseases

Endosomal dysfunction in SPG8 parallels mechanisms in^[5]:

• [Parkinson's disease](/diseases/parkinsons-disease): [VPS35](/genes/vps35) mutations cause PD (PARK17); VPS35 directly recruits WASH complex via FAM21
• [Alzheimer's disease](/diseases/alzheimers-disease): Retromer-WASH dysfunction affects [APP](/entities/app-protein) processing and [Aβ](/proteins/amyloid-beta) production
• Other HSPs: [SPAST](/genes/spast) (SPG4), [ATL1](/genes/atl1) (SPG3A), [SPG7](/genes/spg7) share endosomal/ER themes
• [Hao-Fountain syndrome](/genes/usp7): [USP7](/genes/usp7) regulates WASH complex through deubiquitination

Common Variants

| Variant | Effect | Phenotype |
|---------|--------|-----------|
| V626F | Missense | SPG8 (original family) |
| L619F | Missense | SPG8 |
| N471D | Missense | SPG8 |
| E532K | Missense | SPG8 (late onset) |
| R583H | Missense | SPG8 |

Most SPG8 variants are missense mutations clustering in the central region of strumpellin, suggesting this region is critical for WASH complex function or protein interactions^[3].

Expression

WASHC5 is ubiquitously expressed with high levels in the nervous system^[1]:

• Motor [cortex](/brain-regions/cortex): High expression in upper motor neurons (Betz cells)
• Spinal cord: Corticospinal tract neurons
• Cerebral cortex: Broadly expressed in pyramidal neurons
• [Hippocampus](/brain-regions/hippocampus): Moderate expression
• Cerebellum: Purkinje cells
• Peripheral nerves: Motor and sensory neurons

Therapeutic Implications

• Endosomal trafficking enhancers: Compounds that boost WASH-dependent or retromer-mediated recycling
• Chaperone therapy: Stabilizing mutant strumpellin within the WASH complex
• R33 (retromer stabilizer): Pharmacological chaperone for VPS35/retromer that may compensate for WASH complex dysfunction
• Gene therapy: AAV-mediated wild-type WASHC5 delivery (dominant negative mechanism may complicate this approach)

See Also

• [VPS35 Gene](/genes/vps35)
• [SPAST Gene](/genes/spast)
• [Endolysosomal Trafficking Defects](/mechanisms/endolysosomal-trafficking-defects)
• [USP7 Gene](/genes/usp7)
• [Hereditary Spastic Paraplegia](/diseases/hereditary-spastic-paraplegia)

External Links

• [WASHC5 - NCBI Gene](https://www.ncbi.nlm.nih.gov/gene/9744)
• [WASHC5 - UniProt](https://www.uniprot.org/uniprot/Q12768)
• [SPG8 - OMIM](https://omim.org/entry/603563)

References