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  • The autophagy/lysosome pathway is impaired in SCA7 patients and SCA7 knock-in mice.

The autophagy/lysosome pathway is impaired in SCA7 patients and SCA7 knock-in mice.

Acta neuropathologica (2014-05-27)
Sandro Alves, Florence Cormier-Dequaire, Martina Marinello, Thibaut Marais, Marie-Paule Muriel, Florian Beaumatin, Fanny Charbonnier-Beaupel, Khadija Tahiri, Danielle Seilhean, Khalid El Hachimi, Merle Ruberg, Giovanni Stevanin, Martine Barkats, Wilfred den Dunnen, Muriel Priault, Alexis Brice, Alexandra Durr, Jean-Christophe Corvol, Annie Sittler
ABSTRACT

There is still no treatment for polyglutamine disorders, but clearance of mutant proteins might represent a potential therapeutic strategy. Autophagy, the major pathway for organelle and protein turnover, has been implicated in these diseases. To determine whether the autophagy/lysosome system contributes to the pathogenesis of spinocerebellar ataxia type 7 (SCA7), caused by expansion of a polyglutamine tract in the ataxin-7 protein, we looked for biochemical, histological and transcriptomic abnormalities in components of the autophagy/lysosome pathway in a knock-in mouse model of the disease, postmortem brain and peripheral blood mononuclear cells (PBMC) from patients. In the mouse model, mutant ataxin-7 accumulated in inclusions immunoreactive for the autophagy-associated proteins mTOR, beclin-1, p62 and ubiquitin. Atypical accumulations of the autophagosome/lysosome markers LC3, LAMP-1, LAMP2 and cathepsin-D were also found in the cerebellum of the SCA7 knock-in mice. In patients, abnormal accumulations of autophagy markers were detected in the cerebellum and cerebral cortex of patients, but not in the striatum that is spared in SCA7, suggesting that autophagy might be impaired by the selective accumulation of mutant ataxin-7. In vitro studies demonstrated that the autophagic flux was impaired in cells overexpressing full-length mutant ataxin-7. Interestingly, the expression of the early autophagy-associated gene ATG12 was increased in PBMC from SCA7 patients in correlation with disease severity. These results provide evidence that the autophagy/lysosome pathway is impaired in neurons undergoing degeneration in SCA7. Autophagy/lysosome-associated molecules might, therefore, be useful markers for monitoring the effects of potential therapeutic approaches using modulators of autophagy in SCA7 and other autophagy/lysosome-associated neurodegenerative disorders.