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Impact of Prenatal and Subsequent Adult Alcohol Exposure on Pro-Inflammatory Cytokine Expression in Brain Regions Necessary for Simple Recognition Memory

机译:产前和以后的成人酒精暴露对简单识别记忆所必需的大脑区域促炎性细胞因子表达的影响

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摘要

Microglia, the immune cells of the brain, are important and necessary for appropriate neural development; however, activation of microglia, concomitant with increased levels of secreted immune molecules during brain development, can leave the brain susceptible to certain long-term changes in immune function associated with neurological and developmental disorders. One mechanism by which microglia can be activated is via alcohol exposure. We sought to investigate if low levels of prenatal alcohol exposure can alter the neuroimmune response to a subsequent acute dose of alcohol in adulthood. We also used the novel object location and recognition memory tasks to determine whether there are cognitive deficits associated with low prenatal alcohol exposure and subsequent adulthood alcohol exposure. We found that adult rats exposed to an acute binge-like level of alcohol, regardless of gestational alcohol exposure, have a robust increase in the expression of Interleukin (IL)-6 within the brain, and a significant decrease in the expression of IL-1β and CD11b. Rats exposed to alcohol during gestation, adulthood, or at both time points exhibited impaired cognitive performance in the cognitive tasks. These results indicate that both low-level prenatal alcohol exposure and even acute alcohol exposure in adulthood can significantly impact neuroimmune and associated cognitive function.
机译:小胶质细胞是大脑的免疫细胞,对于适当的神经发育非常重要和必要。然而,小胶质细胞的激活伴随着大脑发育过程中分泌的免疫分子水平的增加,可能使大脑容易受到与神经系统和发育障碍有关的免疫功能的某些长期变化的影响。可以激活小胶质细胞的一种机制是通过酒精暴露。我们试图研究低水平的产前酒精暴露是否可以改变成年后对急性酒精剂量的神经免疫反应。我们还使用了新颖的对象定位和识别记忆任务来确定是否存在与低产前酒精暴露和随后的成年酒精暴露相关的认知缺陷。我们发现,暴露于急性暴饮性酒精水平的成年大鼠,无论孕期酒精暴露如何,其脑内白介素(IL)-6的表达均呈强劲增加,而IL--6的表达则明显降低。 1β和CD11b。在妊娠期,成年期或两个时间点都暴露于酒精的大鼠在认知任务中表现出受损的认知能力。这些结果表明,成年期低水平的产前酒精暴露甚至急性酒精暴露都可以显着影响神经免疫和相关的认知功能。

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