阿波啡激活老年痴呆模型5XFAD转基因小鼠多巴胺能系统后的基线脑电图及其演化

V. Vorobyov, Alexander Deev, Zoya Oganesyan, F. Sengpiel, A. Ustyugov
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引用次数: 1

摘要

衰老和阿尔茨海默病(AD)的特征是与神经元连接改变相关的共同病理特征。这些不可避免地影响特定大脑区域的功能及其相互关系,导致有关神经元可塑性和多巴胺能(DA)调解相关的代偿机制的问题。本研究以12月龄自由活动的5xfad转基因小鼠作为AD模型,及其野生型(WT)仔鼠为实验对象,分析了运动皮质(MC)、壳核(Pt)、产生da的腹侧被盖区(VTA)和黑质(SN)的脑电图(eeg)。转基因小鼠的基线脑电图表现为VTA区δ 2活性增强,VTA和SN区α活性减弱。与WT小鼠相比,这些脑区的脑电图没有差异,5XFAD小鼠在VTA和SN与MC的脑电图中表现出α - α衰减,δ 2和β 2增强。在5XFAD小鼠中,模拟DA的阿波啡降低了(相对于生理盐水)Pt、VTA和SN的θ振荡,增强了MC、Pt、VTA和β 1在所有脑区的α。这些结果以及早期在幼龄(6个月)小鼠中获得的结果表明,AD影响的大脑适应机制的年龄相关特征可能与不同脑区间动态相互关系机制中多巴胺能介导的改变有关。
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Baseline Electroencephalogram and Its Evolution after Activation of Dopaminergic System by Apomorphine in Middle-Aged 5XFAD Transgenic Mice, a Model of Alzheimer’s Disease
Aging and Alzheimer’s disease (AD) are characterized by common pathological features associated with alterations in neuronal connections. These inevitably affect the functioning of specific brain areas and their interrelations, leading to questions about neuronal plasticity and the compensatory mechanisms associated with dopaminergic (DA) mediation. In this study on twelve-month-old freely moving 5XFAD-transgenic mice, serving as a model of AD, and their wild-type (WT) littermates, we analyze electroencephalograms (EEGs) from the motor cortex (MC), putamen (Pt) and the DA-producing ventral tegmental area (VTA) and substantia nigra (SN). Baseline EEGs in the transgenic mice were characterized by delta 2 activity enhancements in VTA and alpha attenuation in VTA and SN. In contrast to WT mice, which lack differences in EEG from these brain areas, 5XFAD mice showed theta–alpha attenuation and delta 2 and beta 2 enhancements in EEG from both VTA and SN vs. MC. In 5XFAD mice, a DA mimetic, apomorphine, lowered (vs. saline) the theta oscillations in Pt, VTA and SN and enhanced alpha in MC, Pt, VTA and beta 1 in all brain areas. These results and those obtained earlier in younger (six-month-old) mice suggest that the age-related characteristics of cerebral adaptive mechanisms affected by AD might be associated with modification of dopaminergic mediation in the mechanisms of intracerebral dynamic interrelations between different brain areas.
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