CONVERGENT ROLE OF DENTATE GYRUS GRANULE CELLS IN TEMPORAL LOBE EPILEPSY AND AUTISM
Nencki Institute of Experimental Biology PAS
Presentation
Date TBA
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Poster Board
PS06-09PM-114
Poster
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In human patients mutations in PTEN (negative regulator of PI3K–AKT–mTOR signaling) or FMR1 gene (Fragile X Messenger Ribonucleoprotein 1) are critically attributed to ASD. In this study, using mouse models and viral gene transfer we examined whether downregulation of either PTEN or Fmr1 gene selectively in adult DG granule cells is sufficient to evoke mTLE and social memory impairments. Animals with either PTEN-deficient or Fmr1-deficient DG granule cells developed chronic seizures reminiscent to those found in patients with mTLE. In addition, PTEN mutants demonstrated impaired interaction in bilateral social contact with conspecifics as well as strong hierarchy instability in cohort studies. While adequate social memory tests on Fmr1 mutants are pending, described results indicate that DG granule cells define a shared circuit mechanism for mTLE and ASD related social memory deficits.
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