![Fig. 2. Abnormal memory of the context a day after training on the fear-conditioning paradigm. (A) Percent of freezing in a 5-min session of fear conditioning , on cue test [2 h (diploid: n = 8, triploid: n = 6), 26 h (n = 8 for each group) and 7 d posttraining (n = 7 for each group)] and context test [24 h (diploid: n = 8, triploid: n = 6) and 7 d posttraining)]. (B) Percent of freezing on the context test a day after training in bins of 30 s. *P < 0.05.](https://www.researchgate.net/profile/Liora-Guy-David/publication/221808830/figure/fig2/AS:349422748749829@1460320283607/Abnormal-memory-of-the-context-a-day-after-training-on-the-fear-conditioning-paradigm_Q320.jpg)
February 2012
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74 Citations
Proceedings of the National Academy of Sciences
G protein-activated inwardly rectifying K+ channels (GIRK) generate slow inhibitory postsynaptic potentials in the brain via G(i/o) protein-coupled receptors. GIRK2, a GIRK subunit, is widely abundant in the brain and has been implicated in various functions and pathologies, such as learning and memory, reward, motor coordination, and Down syndrome. Down syndrome, the most prevalent cause of mental retardation, results from the presence of an extra maternal chromosome 21 (trisomy 21), which comprises the Kcnj6 gene (GIRK2). The present study examined the behaviors and cellular physiology properties in mice harboring a single trisomy of the Kcnj6 gene. Kcnj6 triploid mice exhibit deficits in hippocampal-dependent learning and memory, altered responses to rewards, hampered depotentiation, a form of excitatory synaptic plasticity, and have accentuated long-term synaptic depression. Collectively the findings suggest that triplication of Kcnj6 gene may play an active role in some of the abnormal neurological phenotypes found in Down syndrome.
