PEX10 Protein

PEX10 Protein

Overview

PEX10 (Peroxisomal Biogenesis Factor 10) is an integral peroxisomal membrane protein that plays a critical role in peroxisomal assembly and protein import. The PEX10 gene, located on chromosome 1q22, encodes a 35-kDa RING-type E3 ubiquitin ligase that functions as a key component of the peroxisomal docking and translocation machinery. PEX10 belongs to the family of PEX (peroxisome biogenesis factor) proteins, which are essential for the biogenesis and maintenance of functional peroxisomes. Mutations in PEX10 cause Zellweger spectrum disorders (ZSD), a group of severe autosomal recessive conditions characterized by peroxisomal dysfunction. Beyond its classical role in peroxisomal biogenesis, emerging evidence suggests PEX10 dysfunction contributes to neurodegeneration through mechanisms involving impaired protein quality control and accumulation of toxic lipid species.

Function/Biology

PEX10 functions as a component of the peroxisomal import machinery, where it works in conjunction with other PEX proteins to facilitate the translocation of cargo proteins into the peroxisomal matrix. The protein contains a conserved RING (Really Interesting New Gene) motif that possesses E3 ubiquitin ligase activity, enabling it to catalyze the conjugation of ubiquitin to target proteins. PEX10 is anchored to the peroxisomal membrane through transmembrane domains and interacts with multiple PEX proteins, including PEX5, PEX12, and PEX1, forming the receptor-docking and ubiquitination complex.

PEX10 Protein

Overview

PEX10 (Peroxisomal Biogenesis Factor 10) is an integral peroxisomal membrane protein that plays a critical role in peroxisomal assembly and protein import. The PEX10 gene, located on chromosome 1q22, encodes a 35-kDa RING-type E3 ubiquitin ligase that functions as a key component of the peroxisomal docking and translocation machinery. PEX10 belongs to the family of PEX (peroxisome biogenesis factor) proteins, which are essential for the biogenesis and maintenance of functional peroxisomes. Mutations in PEX10 cause Zellweger spectrum disorders (ZSD), a group of severe autosomal recessive conditions characterized by peroxisomal dysfunction. Beyond its classical role in peroxisomal biogenesis, emerging evidence suggests PEX10 dysfunction contributes to neurodegeneration through mechanisms involving impaired protein quality control and accumulation of toxic lipid species.

Function/Biology

PEX10 functions as a component of the peroxisomal import machinery, where it works in conjunction with other PEX proteins to facilitate the translocation of cargo proteins into the peroxisomal matrix. The protein contains a conserved RING (Really Interesting New Gene) motif that possesses E3 ubiquitin ligase activity, enabling it to catalyze the conjugation of ubiquitin to target proteins. PEX10 is anchored to the peroxisomal membrane through transmembrane domains and interacts with multiple PEX proteins, including PEX5, PEX12, and PEX1, forming the receptor-docking and ubiquitination complex.

The primary function of PEX10 involves the ubiquitination of peroxisomal targeting signal (PTS) receptors, particularly PEX5 and PEX7, which recognize and bind cargo proteins destined for peroxisomes. This ubiquitination process marks these receptors for extraction from the peroxisomal membrane and subsequent recycling via the proteasomal pathway. This cycling of receptors is essential for the continuous transport of peroxisomal matrix proteins. Additionally, PEX10 participates in the Quality Control of peroxisomal proteins and helps maintain the structural integrity of the peroxisomal membrane.

Role in Neurodegeneration

PEX10 dysfunction is implicated in neurodegeneration through multiple pathways related to peroxisomal failure. Peroxisomes are essential for fatty acid β-oxidation, particularly the degradation of very long-chain fatty acids (VLCFAs), and for the synthesis of plasmalogens, lipids critical for myelin formation and neuronal membrane integrity. When PEX10 is defective or absent, peroxisomes cannot properly import and process these functions, leading to toxic accumulation of VLCFAs and reduced plasmalogen synthesis.

The accumulation of VLCFAs and their metabolic byproducts creates oxidative stress within neurons and oligodendrocytes, triggering neuroinflammation and neuronal death. Furthermore, impaired plasmalogen synthesis compromises myelin stability and neuronal membrane structure, contributing to progressive neurological deterioration. The cerebellar and spinal cord pathologies observed in Zellweger spectrum disorders reflect particular vulnerability of these regions to peroxisomal dysfunction.

Molecular Mechanisms

At the molecular level, PEX10 dysfunction triggers neurodegeneration through several interconnected mechanisms. Loss of PEX10 function prevents proper ubiquitination and recycling of PEX5 and PEX7 receptors, causing accumulation of these proteins at the peroxisomal membrane and impairing cargo import. This disruption leads to substrate accumulation outside peroxisomes and failure to complete essential metabolic pathways.

The impaired degradation of VLCFAs results in their accumulation in all tissues, with particular accumulation in myelin-forming oligodendrocytes and neuronal axons. Elevated VLCFA levels generate reactive oxygen species (ROS) through enhanced peroxisomal and mitochondrial oxidation, activating apoptotic cascades. Additionally, defective plasmalogen synthesis reduces the antioxidant capacity of neuronal membranes, exacerbating oxidative damage.

PEX10 mutations also compromise autophagy-dependent removal of dysfunctional peroxisomes, leading to accumulation of damaged organelles and enhanced cellular stress. This impaired mitophagy and pexophagy subsequently affects mitochondrial function and energy metabolism in neurons.

Clinical/Research Significance

PEX10 mutations represent approximately 20-30% of Zellweger spectrum disorder cases, making it one of the most frequently mutated genes in peroxisomal biogenesis disorders. Clinical manifestations range from neonatal adrenoleukodystrophy (NALD) to infantile Refsum disease (IRD), with severity depending on residual PEX10 function. Research into PEX10 has implications for understanding peroxisomal involvement in other neurodegenerative conditions and for developing therapeutic strategies targeting peroxisomal restoration.