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Systemic inflammation enhances stimulant-induced striatal dopamine elevation

机译:全身性炎症会加剧兴奋剂引起的纹状体多巴胺升高

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摘要

Changes in the mesolimbic dopamine (DA) system are implicated in a range of neuropsychiatric conditions including addiction, depression and schizophrenia. Dysfunction of the neuroimmune system is often comorbid with such conditions and affects similar areas of the brain. The goal of this study was to use positron emission tomography with the dopamine D2 antagonist tracer, 11C-raclopride, to explore the effect of acute immune activation on striatal DA levels. DA transmission was modulated by an oral methylphenidate (MP) challenge in order to reliably elicit DA elevation. Elevation in DA concentration due to MP was estimated via change in 11C-raclopride binding potential from the baseline scan. Prior to the post-MP scan, subjects were pre-treated with either the immune activator lipopolysaccharide (LPS) or placebo (PBO) in a cross-over design. Immune activation was confirmed by measuring tumor necrosis factor alpha (TNFα), interleukin (IL)-6 and IL-8 concentration in plasma. Eight healthy subjects were scanned four times each to determine the MP-induced DA elevation under both LPS and PBO pre-treatment conditions. MP-induced DA elevation in the striatum was significantly greater (P<0.01) after LPS pre-treatment compared to PBO pre-treatment. Seven of eight subjects responded similarly. This effect was observed in the caudate and putamen (P<0.02), but was not present in ventral striatum. DA elevation induced by MP was significantly greater when subjects were pre-treated with LPS compared to PBO. The amplification of stimulant-induced DA signaling in the presence of systemic inflammation may have important implications for our understanding of addiction and other diseases of DA dysfunction.
机译:中脑边缘多巴胺(DA)系统的变化与成瘾,抑郁和精神分裂症等一系列神经精神疾病有关。神经免疫系统的功能障碍通常与此类疾病并存,并影响大脑的类似区域。这项研究的目的是将正电子发射断层扫描与多巴胺D2拮抗剂示踪剂 11 C-雷洛必利一起使用,以探讨急性免疫激活对纹状体DA水平的影响。为了可靠地引起DA升高,口服哌醋甲酯(MP)刺激调节了DA的传播。通过基线扫描中 11 C-雷洛必利结合潜力的变化来估计由于MP引起的DA浓度升高。在MP后扫描之前,以交叉设计对受试者进行免疫激活剂脂多糖(LPS)或安慰剂(PBO)预处理。通过测量血浆中的肿瘤坏死因子α(TNFα),白介素(IL)-6和IL-8浓度来确认免疫激活。对八个健康受试者进行了四次扫描,以确定在LPS和PBO预处理条件下MP诱导的DA升高。与PBO预处理相比,LPS预处理后MP诱导的纹状体DA升高明显更高(P <0.01)。八名受试者中有七名做出类似反应。在尾状和壳状核中观察到这种作用(P <0.02),但在腹侧纹状体中不存在。与PBO相比,LPS预处理的受试者MP引起的DA升高明显更大。在全身性炎症的存在下,兴奋剂诱导的DA信号的扩增可能对我们对成瘾和其他DA功能障碍疾病的理解具有重要意义。

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