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Publication : Dystonia and cerebellar degeneration in the leaner mouse mutant.

First Author  Raike RS Year  2015
Journal  Brain Res Volume  1611
Pages  56-64 PubMed ID  25791619
Mgi Jnum  J:221960 Mgi Id  MGI:5643797
Doi  10.1016/j.brainres.2015.03.011 Citation  Raike RS, et al. (2015) Dystonia and cerebellar degeneration in the leaner mouse mutant. Brain Res 1611:56-64
abstractText  Cerebellar degeneration is traditionally associated with ataxia. Yet, there are examples of both ataxia and dystonia occurring in individuals with cerebellar degeneration. There is also substantial evidence suggesting that cerebellar dysfunction alone may cause dystonia. The types of cerebellar defects that may cause ataxia, dystonia, or both have not been delineated. In the current study, we explored the relationship between cerebellar degeneration and dystonia using the leaner mouse mutant. Leaner mice have severe dystonia that is associated with dysfunctional and degenerating cerebellar Purkinje cells. Whereas the density of Purkinje cells was not significantly reduced in 4 week-old leaner mice, approximately 50% of the neurons was lost by 34 weeks of age. On the other hand, the dystonia and associated functional disability became significantly less severe during this same interval. In other words, dystonia improved as Purkinje cells were lost, suggesting that dysfunctional Purkinje cells, rather than Purkinje cell loss, contribute to the dystonia. These results provide evidence that distorted cerebellar function may cause dystonia and support the concept that different types of cerebellar defects can have different functional consequences.
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