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Neurobiological Correlates of Individual Differences in Novelty-Seeking Behavior in the Rat: Differential Expression of Stress-Related Molecules

机译:大鼠寻求新奇行为的个体差异的神经生物学相关性:应激相关分子的差异表达。

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摘要

It is well established that individual rats exhibit marked differences in behavioral responses to a novel environment. Rats that exhibit high rates of locomotor activity and sustained exploration in such an environment also exhibit high concentrations of stress-induced plasma corticosterone, linking this behavior to the stress system. Furthermore, these high-responding (HR) rats, in contrast to their low-responding (LR) counterparts, have a greater propensity to self-administer drugs. Thus, HR rats have been described as “novelty” seeking in that they are more active and explore novel stimuli more vigorously, despite the fact that this elicits in them high stress responses. In this study, we have further characterized the behavior of HR and LR rats in tests of anxiety and characterized their stress responses to either experimenter- or self-imposed stressors. We then investigated the physiological basis of these individual differences, focusing on stress-related molecules, including the glucocorticoid receptor (GR), the mineralocorticoid receptor (MR), corticotropin-releasing hormone (CRH) and pro-opiomelanocortin (POMC) in the context of the limbic–hypothalamo–pituitary adrenal axis. We have found that HR rats did not differ from LR in their basal expression of POMC in the pituitary. However, HR rats exhibited higher levels of CRH mRNA in the hypothalamic paraventricular nucleus but lower basal levels in the central nucleus of the amygdala. The basal expression of hippocampal MR is not different between HR and LR rats. Interestingly, the basal expression of hippocampal GR mRNA is significantly lower in HR than in LR rats. This low level of hippocampal GR expression in HR rats appears to be responsible, at least in part, for their decreased anxiety in exploring novelty. Indeed, the anxiety level of LR rats becomes similar to HR rats after the administration into the hippocampus of a GR antagonist, RU38486. These data indicate that basal differences in gene expression of key stress-related molecules may play an important role in determining individual differences in responsiveness to stress and novelty. They point to a new role of hippocampal GR, strongly implicating this receptor in determining individual differences in anxiety and novelty-seeking behavior.
机译:公认的是,个别大鼠在对新环境的行为反应中表现出明显的差异。在这样的环境中表现出高运动能力和持续探索的大鼠也表现出高浓度的应激诱导血浆皮质酮,将这种行为与应激系统联系起来。此外,与低响应(LR)的对立相比,这些高响应(HR)的大鼠具有更大的自我给药倾向。因此,HR大鼠被描述为“新颖”寻求者,因为它们更加活跃,并且更加积极地探索新的刺激,尽管事实上这会在它们中引起高压力反应。在这项研究中,我们进一步表征了HR和LR大鼠在焦虑测试中的行为,并表征了它们对实验者或自我施加的应激源的应激反应。然后,我们研究了这些个体差异的生理基础,重点研究了与压力相关的分子,包括糖皮质激素受体(GR),盐皮质激素受体(MR),促肾上腺皮质激素释放激素(CRH)和促视色素黑皮质激素(POMC)边缘-下丘脑-垂体肾上腺轴。我们已经发现,HR大鼠的垂体中POMC的基础表达与LR没有区别。但是,HR大鼠在下丘脑室旁核中显示较高的CRH mRNA水平,而在杏仁核中枢中显示较低的基础水平。 HR和LR大鼠之间海马MR的基础表达没有差异。有趣的是,HR大鼠海马GR mRNA的基础表达明显低于LR大鼠。 HR大鼠中这种低水平的海马GR表达似乎至少部分是由于它们探索新奇事物时的焦虑减少所致。实际上,在将GR拮抗剂RU38486施用于海马体后,LR大鼠的焦虑水平变得与HR大鼠相似。这些数据表明关键压力相关分子的基因表达的基础差异可能在确定对压力和新奇反应的个体差异中起重要作用。他们指出了海马GR的新作用,强烈暗示该受体在确定焦虑和寻求新奇行为的个体差异方面。

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