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Publication : Neurodegeneration in Lurcher mice occurs via multiple cell death pathways.

First Author  Doughty ML Year  2000
Journal  J Neurosci Volume  20
Issue  10 Pages  3687-94
PubMed ID  10804210 Mgi Jnum  J:62117
Mgi Id  MGI:1858352 Doi  10.1523/JNEUROSCI.20-10-03687.2000
Citation  Doughty ML, et al. (2000) Neurodegeneration in Lurcher mice occurs via multiple cell death pathways. J Neurosci 20(10):3687-94
abstractText  Lurcher (Lc) is a gain-of-function mutation in the delta2 glutamate receptor (GRID2) that results in the cell-autonomous death of cerebellar Purkinje cells in heterozygous lurcher (+/Lc) mice. This in turn triggers the massive loss of afferent granule cells during the first few postnatal weeks. Evidence suggests that the death of Purkinje cells as a direct consequence of GRID2(Lc) activation and the secondary death of granule cells because of target deprivation occur by apoptosis. We have used mice carrying null mutations of both the Bax and p53 genes to examine the roles of these genes in cell loss in lurcher animals. The absence of Bax delayed Purkinje cell death in response to the GRID2(Lc) mutation and permanently rescued the secondary death of granule cells. In contrast, the p53 deletion had no effect on either cell death pathway. Our results demonstrate that target deprivation induces a Bax-dependent, p53-independent cell death response in cerebellar granule cells in vivo. In contrast, Bax plays a minor role in GRID2(Lc)-mediated Purkinje cell death.
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