Systemic HDAC3 inhibition ameliorates impairments in synaptic plasticity caused by simulated galactic cosmic radiation exposure in male mice

•Whole body multi-ion GCR impairs hippocampal-dependent memory updating in males.•Hippocampal LTP is impaired in male mice exposed to whole body multi-ion GCR.•Systemic HDAC3 inhibition reverses GCR-linked impairments in LTP.•HDAC inhibition may provide novel method for ameliorating GCR effects on cognition. Deep space travel presents a number of measurable risks including exposure to a spectrum of radiations of varying qualities, termed galactic cosmic radiation (GCR) that are capable of penetrating the spacecraft, traversing through the body and impacting brain function. Using rodents, studies have reported that exposure to simulated GCR leads to cognitive impairments associated with changes in hippocampus function that can persist as long as one-year post exposure with no sign of recovery. Whether memory can be updated to incorporate new information in mice exposed to GCR is unknown. Further, mechanisms underlying long lasting impairments in cognitive function as a result of GCR exposure have yet to be defined. Here, we examined whether whole body exposure to simulated GCR using 6 ions and doses of 5 or 30 cGy interfered with the ability to update an existing memory or impact hippocampal synaptic plasticity, a cellular mechanism believed to underlie memory processes, by examining long term potentiation (LTP) in acute hippocampal slices from middle aged male mice 3.5–5 months after radiation exposure. Using a modified version of the hippocampus-dependent object location memory task developed by our lab termed “Objects in Updated Locations” (OUL) task we find that GCR exposure impaired hippocampus-dependent memory updating and hippocampal LTP 3.5–5 months after exposure. Further, we find that impairments in LTP are reversed through one-time systemic subcutaneous injection of the histone deacetylase 3 inhibitor RGFP 966 (10 mg/kg), suggesting that long lasting impairments in cognitive function may be mediated at least in part, through epigenetic mechanisms.