1. Spinal muscular atrophy pathogenic mutations impair the axonogenic properties of axonal-survival of motor neuron
- Author
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Denise Locatelli, Veronica Setola, Mineko Terao, Giorgio Battaglia, Enrico Garattini, Francesca Colciaghi, Silvia Capra, Adele Finardi, and Paolo d'Errico
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Tudor domain ,animal diseases ,Survival of motor neuron ,SMN1 ,Spinal muscular atrophy ,Biology ,Motor neuron ,SMA ,medicine.disease ,Biochemistry ,nervous system diseases ,Cellular and Molecular Neuroscience ,medicine.anatomical_structure ,nervous system ,medicine ,Growth cone ,Neuroscience ,Loss function - Abstract
The axonal survival of motor neuron (a-SMN) protein is a truncated isoform of SMN1, the spinal muscular atrophy (SMA) disease gene. a-SMN is selectively localized in axons and endowed with remarkable axonogenic properties. At present, the role of a-SMN in SMA is unknown. As a first step to verify a link between a-SMN and SMA, we investigated by means of over-expression experiments in neuroblastoma-spinal cord hybrid cell line (NSC34) whether SMA pathogenic mutations located in the N-terminal part of the protein affected a-SMN function. We demonstrated here that either SMN1 missense mutations or small intragenic re-arrangements located in the Tudor domain consistently altered the a-SMN capability of inducing axonal elongation in vitro. Mutated human a-SMN proteins determined in almost all NSC34 motor neurons the growth of short axons with prominent morphologic abnormalities. Our data indicate that the Tudor domain is critical in dictating a-SMN function possibly because it is an association domain for proteins involved in axon growth. They also indicate that Tudor domain mutations are functionally relevant not only for FL-SMN but also for a-SMN, raising the possibility that also a-SMN loss of function may contribute to the pathogenic steps leading to SMA.
- Published
- 2012
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