Abstract
Hereditary spastic paraplegia (HSP) comprises a heterogeneous group of neuropathies affecting upper motor neurons and causing progressive gait disorder. Mutations in the gene SPG3A/atlastin-1 (ATL1), encoding a dynamin superfamily member, which utilizes the energy from GTP hydrolysis for membrane tethering and fusion to promote the formation of a highly branched, smooth endoplasmic reticulum (ER), account for approximately 10% of all HSP cases. The continued discovery and characterization of novel disease mutations are crucial for our understanding of HSP pathogenesis and potential treatments. Here, we report a novel disease-causing, in-frame insertion in the ATL1 gene, leading to inclusion of an additional asparagine residue at position 417 (N417ins). This mutation correlates with complex, early-onset spastic quadriplegia affecting all four extremities, generalized dystonia, and a thinning of the corpus callosum. We show using limited proteolysis and FRET-based studies that this novel insertion affects a region in the protein central to intramolecular interactions and GTPase-driven conformational change, and that this insertion mutation is associated with an aberrant prehydrolysis state. While GTPase activity remains unaffected by the insertion, membrane tethering is increased, indicative of a gain-of-function disease mechanism uncommon for ATL1-associated pathologies. In conclusion, our results identify a novel insertion mutation with altered membrane tethering activity that is associated with spastic quadriplegia, potentially uncovering a broad spectrum of molecular mechanisms that may affect neuronal function.
Highlights
Hereditary spastic paraplegias (HSPs) are a heterogenous group of neurodegenerative disorders
We present a case of an early onset, complex HSP caused by a novel ATL1 mutation, where an asparagine residue is inserted into the middle domain between arginine residue and tyrosine residue (N417ins), the first reported clinical case caused by a whole codon insertion in ATL1
Here we have identified a novel mutation in ATL1 that causes a complex form of spastic paraplegia involving all four extremities of the proband
Summary
Hereditary spastic paraplegias (HSPs) are a heterogenous group of neurodegenerative disorders. Investigations into the structure and function of this novel ATL1 variant revealed that does the insertion mutant result in a stable protein, but it preserves many core functions, including GTP hydrolysis and nucleotide-dependent dimerization.
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