Post-exposure environment modulates long-term developmental ethanol effects on behavior, neuroanatomy, and cortical oscillations
•Developmental EtOH exposure has long-lasting effects on sleep physiology.•Post-exposure exercise repaired sleep spindle density in EtOH exposed mice.•Contextual memory and CA1 hippocampal PV+ neuron density also recovered.•EtOH-induced loss of dentate gyrus PV+ cells did not recover. Developmental...
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Veröffentlicht in: | Brain research 2020-12, Vol.1748, p.147128-147128, Article 147128 |
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Sprache: | eng |
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Zusammenfassung: | •Developmental EtOH exposure has long-lasting effects on sleep physiology.•Post-exposure exercise repaired sleep spindle density in EtOH exposed mice.•Contextual memory and CA1 hippocampal PV+ neuron density also recovered.•EtOH-induced loss of dentate gyrus PV+ cells did not recover.
Developmental exposure to ethanol has a wide range of anatomical, cellular, physiological and behavioral impacts that can last throughout life. In humans, this cluster of effects is termed fetal alcohol spectrum disorder and is highly prevalent in western cultures. The ultimate expression of the effects of developmental ethanol exposure however can be influenced by post-exposure experience. Here we examined the effects of developmental binge exposure to ethanol (postnatal day 7) in C57BL/6By mice on a specific cohort of inter-related long-term outcomes including contextual memory, hippocampal parvalbumin-expressing neuron density, frontal cortex oscillations related to sleep-wake cycling including delta oscillation amplitude and sleep spindle density, and home-cage behavioral activity. When assessed in adults that were raised in standard housing, all of these factors were altered by early ethanol exposure compared to saline controls except home-cage activity. However, exposure to an enriched environment and exercise from weaning to postnatal day 90 reversed most of these ethanol-induced impairments including memory, CA1 but not dentate gyrus PV+ cell density, delta oscillations and sleep spindles, and enhanced home-cage behavioral activity in Saline- but not EtOH-treated mice. The results are discussed in terms of the inter-dependence of diverse developmental ethanol outcomes and potential mechanisms of post-exposure experiences to regulate those outcomes. |
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ISSN: | 0006-8993 1872-6240 |
DOI: | 10.1016/j.brainres.2020.147128 |