4.2 Article

Influence of early-life adversity on responses to acute and chronic ethanol in female mice

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ALCOHOL-CLINICAL AND EXPERIMENTAL RESEARCH
卷 47, 期 2, 页码 336-347

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WILEY
DOI: 10.1111/acer.14988

关键词

early-life stress; hyperkatifeia; pain; resilience; vulnerability

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Stressful early-life experiences increase the risk of developing an alcohol use disorder. In this study, it was found that male mice reared under limited bedding and nesting conditions escalated their ethanol intake faster than control mice when exposed to chronic intermittent ethanol inhalation. However, the alcohol consumption of female littermates was not affected by these conditions. This suggests a general insensitivity of female mice to the influence of early-life stress on alcohol responses.
BackgroundStressful early-life experiences increase the risk of developing an alcohol use disorder. We previously found that male C57BL/6J mice reared under limited bedding and nesting (LBN) conditions, a model of early-life adversity, escalate their ethanol intake in limited-access two-bottle choice (2BC) sessions faster than control (CTL)-reared counterparts when exposed to chronic intermittent ethanol (CIE) vapor inhalation. However, the alcohol consumption of female littermates was not affected by LBN or CIE. In the present study, we sought to determine whether this phenotype reflected a general insensitivity of female mice to the influence of early-life stress on alcohol responses. MethodsIn a first experiment, CTL and LBN females with a history of 2BC combined or not with CIE were tested in affective and nociceptive assays during withdrawal. In a second group of CTL and LBN females, we examined ethanol-induced antinociception, sedation, plasma clearance, and c-Fos induction. ResultsIn females withdrawn from chronic 2BC, CIE increased digging, reduced grooming, and increased immobility in the tail suspension test regardless of early-life history. In contrast, LBN rearing lowered mechanical nociceptive thresholds regardless of CIE exposure. In females acutely treated with ethanol, LBN rearing facilitated antinociception and delayed the onset of sedation without influencing ethanol clearance rate or c-Fos induction in the paraventricular nucleus of the hypothalamus, paraventricular nucleus of the thalamus, central nucleus of the amygdala, or auditory cortex. ConclusionCIE withdrawal produced multiple indices of negative affect in C57BL/6J females, suggesting that their motivation to consume alcohol may differ from air-exposed counterparts despite equivalent intake. Contrasted with our previous findings in males, LBN-induced mechanical hyperalgesia in chronic alcohol drinkers was specific to females. Lower nociceptive thresholds combined with increased sensitivity to the acute antinociceptive effect of ethanol may contribute to reinforcing ethanol consumption in LBN females but are not sufficient to increase their intake.

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