Neurobiology of Disease (Apr 2007)

Impaired spatial learning and defective theta burst induced LTP in mice lacking fibroblast growth factor 14

  • David F. Wozniak,
  • Maolei Xiao,
  • Lin Xu,
  • Kelvin A. Yamada,
  • David M. Ornitz

Journal volume & issue
Vol. 26, no. 1
pp. 14 – 26

Abstract

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Spinocerebellar ataxia 27 (SCA27) is a recently described syndrome characterized by impaired cognitive abilities and a slowly progressive ataxia. SCA27 is caused by an autosomal dominant missense mutation in Fibroblast Growth Factor 14 (FGF14). Mice lacking FGF14 (Fgf14−/− mice) have impaired sensorimotor functions, ataxia and paroxysmal dyskinesia, a phenotype that led to the discovery of the human mutation. Here we extend the similarities between Fgf14−/− mice and FGF14(F145S) humans by showing that Fgf14−/− mice exhibit reliable acquisition (place learning) deficits in the Morris water maze. This cognitive deficit appears to be independent of sensorimotor disturbances and relatively selective since Fgf14−/− mice performed similarly to wild type littermates during cued water maze trials and on conditioned fear and passive avoidance tests. Impaired theta burst initiated long-term synaptic potentiation was also found in hippocampal slices from Fgf14−/− mice. These results suggest a role for FGF14 in certain spatial learning functions and synaptic plasticity.

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