Postsymptomatic restoration of SMN rescues the disease phenotype in a mouse model of severe spinal muscular atrophy
Cathleen M. Lutz, Shingo Kariya, Sunita Patruni, Melissa A. Osborne, Don Liu, Christopher E. Henderson, Darrick K. Li, Livio Pellizzoni, José Rojas, David M. Valenzuela, Andrew J. Murphy, Margaret L. Winberg, Umrao R. Monani
Cathleen M. Lutz, Shingo Kariya, Sunita Patruni, Melissa A. Osborne, Don Liu, Christopher E. Henderson, Darrick K. Li, Livio Pellizzoni, José Rojas, David M. Valenzuela, Andrew J. Murphy, Margaret L. Winberg, Umrao R. Monani
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Research Article

Postsymptomatic restoration of SMN rescues the disease phenotype in a mouse model of severe spinal muscular atrophy

Abstract

Spinal muscular atrophy (SMA) is a common neuromuscular disorder in humans. In fact, it is the most frequently inherited cause of infant mortality, being the result of mutations in the survival of motor neuron 1 (SMN1) gene that reduce levels of SMN protein. Restoring levels of SMN protein in individuals with SMA is perceived to be a viable therapeutic option, but the efficacy of such a strategy once symptoms are apparent has not been determined. We have generated mice harboring an inducible Smn rescue allele and used them in a model of SMA to investigate the effects of turning on SMN expression at different time points during the course of the disease. Restoring SMN protein even after disease onset was sufficient to reverse neuromuscular pathology and effect robust rescue of the SMA phenotype. Importantly, our findings also indicated that there was a therapeutic window of opportunity from P4 through P8 defined by the extent of neuromuscular synapse pathology and the ability of motor neurons to respond to SMN induction, following which restoration of the protein to the organism failed to produce therapeutic benefit. Nevertheless, our results suggest that even in severe SMA, timely reinstatement of the SMN protein may halt the progression of the disease and serve as an effective postsymptomatic treatment.

Authors

Cathleen M. Lutz, Shingo Kariya, Sunita Patruni, Melissa A. Osborne, Don Liu, Christopher E. Henderson, Darrick K. Li, Livio Pellizzoni, José Rojas, David M. Valenzuela, Andrew J. Murphy, Margaret L. Winberg, Umrao R. Monani

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Figure 6

Level of phenotypic rescue is inversely correlated with the extent of neuromuscular synapse pathology.

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Level of phenotypic rescue is inversely correlated with the extent of ne...
(A) Immunohistochemistry of cervical spinal cord sections from mice administered TM at various time points during the course of the disease revealed gems (arrows) and normal cytoplasmic staining only in P4-treated mutants. Scale bars: 125 μm and 5 μm (insets). The timing of SMN restoration correlates closely with (B) AChR cluster development as well as (C) the ability to clear presynaptic NF aggregates by P17. Early treatment resulted in greater sophistication of the postsynapse and reduced NF in nerve terminals. *P < 0.05; **P < 0.01; ***P < 0.001; 1-way ANOVA. Note: more than 500 AChR clusters (for postsynaptic specialization) and more than 50 endplates (for NF accumulation) were examined in at least 3 mice per time point. Data are represented as mean ± SEM.