4.7 Article

Sex- and subtype-specific adaptations in excitatory signaling onto deep-layer prelimbic cortical pyramidal neurons after chronic alcohol exposure

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NEUROPSYCHOPHARMACOLOGY
卷 46, 期 11, 页码 1927-1936

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SPRINGERNATURE
DOI: 10.1038/s41386-021-01034-1

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  1. NIAAA [P60-AA011605]
  2. UNC Bowles Center for Alcohol Studies

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Long-term alcohol use leads to behavioral deficits in both male and female rats, with differences in effects observed between sexes. Male rats showed enhanced glutamatergic signaling onto deep-layer principal cells after alcohol exposure, while female rats exhibited improved working memory performance. These findings suggest fundamental differences in alcohol effects on cell activity, cortical sub-circuits, and PFC-dependent behaviors between male and female rats.
Long-term alcohol use results in behavioral deficits including impaired working memory, elevated anxiety, and blunted inhibitory control that is associated with prefrontal cortical (PFC) dysfunction. Preclinical observations demonstrate multiple impairments in GABAergic neurotransmission onto deep-layer principal cells (PCs) in the prelimbic cortex that suggest dependence-related cortical dysfunction is the product of elevated excitability in these cells. Despite accumulating evidence showing alcohol-induced changes in interneuron signaling onto PCs differ between sexes, there is limited data explicitly evaluating sex-specific ethanol effects on excitatory signaling onto deep-layer PCs that may further contribute to deficits in PFC-dependent behaviors. To address this, we conducted electrophysiological and behavioral tests in both male and female Sprague-Dawley rats to evaluate the effects of chronic ethanol exposure. Among our observations, we report a marked enhancement in glutamatergic signaling onto deep-layer PCs in male, but not female, rats after alcohol exposure. This phenomenon was furthermore specific to a sub-class of PC, sub-cortically projecting Type-A cells, and coincided with enhanced anxiety-like behavior, but no observable deficit in working memory. In contrast, female rats displayed alcohol-induced facilitation in working memory performance with no change in expression of anxiety-like behavior. Together, these results suggest fundamental differences in alcohol effects on cell activity, cortical sub-circuits, and PFC-dependent behaviors across male and female rats.

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