性腺激素和性染色体组成对四种核心基因型小鼠的乙醇摄入、偏好和类似复发行为有不同的贡献。
Gonadal hormones and sex chromosome complement differentially contribute to ethanol intake, preference, and relapse-like behaviour in four core genotypes mice.
机构信息
Department of Psychology and Center for Neuroscience and Behavior, Miami University, Oxford, Ohio, USA.
Department of Statistics, Miami University, Oxford, Ohio, USA.
出版信息
Addict Biol. 2022 Sep;27(5):e13222. doi: 10.1111/adb.13222.
Alcohol use and high-risk alcohol drinking behaviours among women are rapidly rising. In rodent models, females typically consume more ethanol (EtOH) than males. Here, we used the four core genotypes (FCG) mouse model to investigate the influence of gonadal hormones and sex chromosome complement on EtOH drinking behaviours. FCG mice were given access to escalating concentrations of EtOH in a two-bottle, 24-h continuous access drinking paradigm to assess consumption and preference. Relapse-like behaviour was measured by assessing escalated intake following repeated cycles of deprivation and re-exposure. Twenty-four-hour EtOH consumption was greater in mice with ovaries (Sry-), relative to those with testes, and in mice with the XX chromosome complement, relative to those with XY sex chromosomes. EtOH preference was higher in XX versus XY mice. For both consumption and preference, the influences of the Sry gene and sex chromosomes were concentration dependent. Escalated intake following repeated cycles of deprivation and re-exposure emerged only in XX mice (vs. XY). Mice with ovaries (Sry- FCG mice and C57BL/6J females) were also found to consume more water than mice with testes. These results demonstrate that aspects of EtOH drinking behaviour may be independently regulated by sex hormones and chromosomes and inform our understanding of the neurobiological mechanisms which contribute to EtOH dependence in male and female mice. Future investigation of the contribution of sex chromosomes to EtOH drinking behaviours is warranted. We used the FCG mouse model to investigate the influence of gonadal hormones and sex chromosome complement on EtOH drinking behaviours, including the alcohol deprivation effect. Escalated intake following repeated cycles of deprivation and re-exposure emerged only in XX mice (vs. XY). These results demonstrate that aspects of EtOH drinking behaviour may be independently regulated by sex hormones and chromosomes.
女性的饮酒和高危饮酒行为正在迅速增加。在啮齿动物模型中,女性通常比男性消耗更多的乙醇(EtOH)。在这里,我们使用四个核心基因型(FCG)小鼠模型来研究性腺激素和性染色体组成对 EtOH 饮酒行为的影响。FCG 小鼠在 24 小时连续双瓶摄取范式中接触递增浓度的 EtOH,以评估消耗和偏好。通过评估剥夺和重新暴露后反复周期中摄取的增加来测量复发样行为。与具有睾丸的小鼠(Sry-)相比,具有卵巢的 FCG 小鼠(Sry-)以及具有 XX 染色体组成的小鼠,相对于具有 XY 性染色体的小鼠,消耗的 EtOH 更多。与 XY 小鼠相比,XX 小鼠的 EtOH 偏好更高。对于消耗和偏好,Sry 基因和性染色体的影响均与浓度有关。只有在 XX 小鼠(而不是 XY 小鼠)中,反复剥夺和重新暴露后摄取量才会增加。具有卵巢的小鼠(Sry- FCG 小鼠和 C57BL/6J 雌性)也被发现比具有睾丸的小鼠消耗更多的水。这些结果表明,EtOH 饮酒行为的某些方面可能独立于性激素和染色体调节,并为我们理解导致雄性和雌性小鼠 EtOH 依赖的神经生物学机制提供了信息。未来需要进一步研究性染色体对 EtOH 饮酒行为的贡献。我们使用 FCG 小鼠模型来研究性腺激素和性染色体组成对 EtOH 饮酒行为的影响,包括酒精剥夺效应。只有在 XX 小鼠(而不是 XY 小鼠)中,反复剥夺和重新暴露后摄取量才会增加。这些结果表明,EtOH 饮酒行为的某些方面可能独立于性激素和染色体调节。
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