AI Article Synopsis
- The Purkinje cell degeneration (pcd) mouse model represents a genetic condition that leads to rapid loss of cerebellum and retina neurons, primarily Purkinje cells.
- The cause of pcd is linked to the malfunction of the Nna1 gene, a conserved zinc carboxypeptidase, which was studied alongside its Drosophila counterpart, NnaD, to understand the disease.
- Investigations showed that loss of Nna1 function disrupts mitochondrial function and bioenergetics, affecting the expression of specific enzymes vital for energy production.
Article Abstract
The Purkinje cell degeneration (pcd) mouse is a recessive model of neurodegeneration, involving cerebellum and retina. Purkinje cell death in pcd is dramatic, as >99% of Purkinje neurons are lost in 3 weeks. Loss of function of Nna1 causes pcd, and Nna1 is a highly conserved zinc carboxypeptidase. To determine the basis of pcd, we implemented a two-pronged approach, combining characterization of loss-of-function phenotypes of the Drosophila Nna1 ortholog (NnaD) with proteomics analysis of pcd mice. Reduced NnaD function yielded larval lethality, with survivors displaying phenotypes that mirror disease in pcd. Quantitative proteomics revealed expression alterations for glycolytic and oxidative phosphorylation enzymes. Nna proteins localize to mitochondria, loss of NnaD/Nna1 produces mitochondrial abnormalities, and pcd mice display altered proteolytic processing of Nna1 interacting proteins. Our studies indicate that Nna1 loss of function results in altered bioenergetics and mitochondrial dysfunction.
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| http://www.ncbi.nlm.nih.gov/pmc/articles/PMC3101252 | PMC |
| http://dx.doi.org/10.1016/j.neuron.2010.05.024 | DOI Listing |
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