Department of Neurobiology, Duke University Medical Center, Bryan Research Building, Durham, NC 27710, USA.
Neuroscience. 2012 Apr 5;207:167-81. doi: 10.1016/j.neuroscience.2012.01.027. Epub 2012 Jan 21.
Early-life stress has been shown to increase susceptibility to anxiety and substance abuse. Disrupted activity within the anterior insular cortex (AIC) has been shown to play a role in both of these disorders. Altered serotonergic processing is implicated in controlling the activity levels of the associated cognitive networks. We therefore investigated changes in both serotonin receptor expression and glutamatergic synaptic activity in the AIC of alcohol-drinking rhesus monkeys. We studied tissues from male rhesus monkeys raised under two conditions: Male rhesus monkeys (1) "mother reared" (MR) by adult females (n=9) or (2) "Nursery reared" (NR), that is, separated from their mothers and reared as a separate group under surrogate/peer-reared conditions (n=9). The NR condition represents a long-standing and well-validated nonhuman primate model of early life stress. All monkeys were trained to self-administer ethanol (4% w/v) or an isocaloric maltose-dextrin control solution. Subsets from each rearing condition were then given daily access to ethanol, water, or maltose-dextrin for 12 months. Tissues were collected at necropsy and were further analyzed. Using real time RT-PCR we found that ethanol-naive, NR monkeys had lower AIC levels of 5-HT(1A) and 5-HT(2A) receptor mRNA compared with ethanol-naive, MR animals. Although NR monkeys consumed more ethanol over the 12-month period compared with MR animals, both MR and NR animals expressed greater 5-HT(1A) and 5-HT(2A) receptor mRNA levels following chronic alcohol self-administration. The interaction between nursery-rearing conditions and alcohol consumption resulted in a significant enhancement of both 5-HT(1A) and 5-HT(2A) receptor mRNA levels such that lower expression levels observed in nursery-rearing conditions were not found in the alcohol self-administration group. Using voltage clamp recordings in the whole cell configuration we recorded excitatory postsynaptic currents in both ethanol-naive and chronic self-administration groups of NR and MR monkeys. Both groups that self-administered ethanol showed greater glutamatergic activity within the AIC. This AIC hyperactivity in MR alcohol-consuming monkeys was accompanied by an increased sensitivity to regulation by presynaptic 5-HT(1A) receptors that was not apparent in the ethanol-naive, MR group. Our data indicate that chronic alcohol consumption leads to greater AIC activity and may indicate a compensatory upregulation of presynaptic 5-HT(1A) receptors. Our results also indicate that AIC activity may be less effectively regulated by 5-HT in ethanol-naive NR animals than in NR monkeys in response to chronic ethanol self-administration. These data suggest possible mechanisms for increased alcohol seeking and possible addiction potential among young adults who had previously experienced early-life stress that include disruptions in both AIC activity and serotonin system dynamics.
早期生活压力已被证明会增加焦虑和药物滥用的易感性。前岛叶皮层(AIC)内活动的中断被证明在这两种疾病中都起着作用。改变 5-羟色胺能处理与相关认知网络的活动水平有关。因此,我们研究了酒精饮用恒河猴 AIC 中 5-羟色胺受体表达和谷氨酸能突触活性的变化。我们研究了在两种条件下饲养的雄性恒河猴的组织:(1)由成年雌性饲养的“母亲饲养”(MR)(n=9)或(2)“托儿所饲养”(NR),即与母亲分开并在替代/同伴饲养条件下作为单独一组饲养(n=9)。NR 条件代表了一种长期存在且经过充分验证的非人类灵长类动物早期生活压力模型。所有猴子都经过训练以自我给予乙醇(4%w/v)或等热量麦芽糖糊精对照溶液。然后,从每个饲养条件中取出亚组,每天给予乙醇、水或麦芽糖糊精 12 个月。在尸检时收集组织,并进一步进行分析。通过实时 RT-PCR,我们发现与乙醇-naive、MR 动物相比,NR 猴子的 AIC 中 5-HT(1A)和 5-HT(2A)受体 mRNA 水平较低。尽管 NR 猴子在 12 个月期间比 MR 动物消耗更多的乙醇,但在慢性酒精自我给药后,MR 和 NR 动物均表达了更高水平的 5-HT(1A)和 5-HT(2A)受体 mRNA。托儿所饲养条件与酒精消费之间的相互作用导致 5-HT(1A)和 5-HT(2A)受体 mRNA 水平显著增强,因此在酒精自我给药组中未发现托儿所饲养条件下观察到的较低表达水平。使用全细胞膜片钳记录,我们记录了 NR 和 MR 猴子中乙醇-naive 和慢性自我给药组的兴奋性突触后电流。自我给予乙醇的两组均显示 AIC 内谷氨酸能活性增加。在 MR 酒精消耗猴子中,这种 AIC 过度活跃伴随着 5-HT(1A)受体的前突触调节敏感性增加,而在乙醇-naive、MR 组中则不明显。我们的数据表明,慢性酒精消耗会导致 AIC 活动增加,并且可能表明 5-HT1A 受体的前突触上调是一种代偿性反应。我们的结果还表明,与慢性乙醇自我给药相比,NR 猴子中 AIC 活动对 5-HT 的调节可能不太有效,而在乙醇-naiveNR 动物中则不是。这些数据表明,在经历过早期生活压力的年轻人中,可能会出现更高的酒精寻求和可能的成瘾潜力,其中包括 AIC 活动和 5-羟色胺系统动力学的中断。
