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Publication : FXR1P limits long-term memory, long-lasting synaptic potentiation, and de novo GluA2 translation.

First Author  Cook D Year  2014
Journal  Cell Rep Volume  9
Issue  4 Pages  1402-1416
PubMed ID  25456134 Mgi Jnum  J:218753
Mgi Id  MGI:5618352 Doi  10.1016/j.celrep.2014.10.028
Citation  Cook D, et al. (2014) FXR1P limits long-term memory, long-lasting synaptic potentiation, and de novo GluA2 translation. Cell Rep 9(4):1402-16
abstractText  Translational control of mRNAs allows for rapid and selective changes in synaptic protein expression that are required for long-lasting plasticity and memory formation in the brain. Fragile X Related Protein 1 (FXR1P) is an RNA-binding protein that controls mRNA translation in nonneuronal cells and colocalizes with translational machinery in neurons. However, its neuronal mRNA targets and role in the brain are unknown. Here, we demonstrate that removal of FXR1P from the forebrain of postnatal mice selectively enhances long-term storage of spatial memories, hippocampal late-phase long-term potentiation (L-LTP), and de novo GluA2 synthesis. Furthermore, FXR1P binds specifically to the 5' UTR of GluA2 mRNA to repress translation and limit the amount of GluA2 that is incorporated at potentiated synapses. This study uncovers a mechanism for regulating long-lasting synaptic plasticity and spatial memory formation and reveals an unexpected divergent role of FXR1P among Fragile X proteins in brain plasticity.
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