唐氏综合征 Ts65Dn 小鼠模型中海马活动的超刚性阶段性组织,但 CA1 位置细胞的空间特性正常。
Hyper-Rigid Phasic Organization of Hippocampal Activity But Normal Spatial Properties of CA1 Place Cells in the Ts65Dn Mouse Model of Down Syndrome.
机构信息
Department of Anatomy, University of Otago, Dunedin, New Zealand, 9016
Discipline of Pharmacology and Therapeutics, National University of Ireland, Galway, Galway, Ireland, H91 TK33.
出版信息
J Neurosci. 2022 Feb 23;42(8):1542-1556. doi: 10.1523/JNEUROSCI.2636-20.2021. Epub 2022 Jan 3.
Down syndrome (DS) in humans is caused by trisomy of chromosome 21 and is marked by prominent difficulties in learning and memory. Decades of research have demonstrated that the hippocampus is a key structure in learning and memory, and recent work with mouse models of DS has suggested differences in hippocampal activity that may be the substrate of these differences. One of the primary functional differences in DS is thought to be an excess of GABAergic innervation from medial septum to the hippocampus. In these experiments, we probe in detail the activity of region CA1 of the hippocampus using electrophysiology in male Ts65Dn mice compared with their male nontrisomic 2N littermates. We find the spatial properties of place cells in CA1 are normal in Ts65Dn animals. However, we find that the phasic relationship of both CA1 place cells and gamma rhythms to theta rhythm in the hippocampus is profoundly altered in these mice. Since the phasic organization of place cell activity and gamma oscillations on the theta wave are thought to play a critical role in hippocampal function, the changes we observe agree with recent findings that organization of the hippocampal network is potentially of more relevance to its function than the spatial properties of place cells. Recent evidence has disrupted the view that spatial deficits are associated with place cell abnormalities. In these experiments, we record hippocampal place cells and local field potential from the Ts65Dn mouse model of Down syndrome, and find phenomenologically normal place cells, but profound changes in the association of place cells and gamma rhythms with theta rhythm, suggesting that the overall network state is critically important for hippocampal function. These findings also agree with evidence suggesting that excess inhibitory control is the cause of hippocampal dysfunction in Down syndrome. The findings also confirm new avenues for pharmacological treatment of Down syndrome.
唐氏综合征(DS)是由 21 号染色体三体引起的,其特征是学习和记忆方面的明显障碍。几十年来的研究表明,海马体是学习和记忆的关键结构,而最近对 DS 小鼠模型的研究表明,海马体活动存在差异,这可能是这些差异的基础。DS 的主要功能差异之一被认为是来自内侧隔核到海马体的 GABA 能神经支配过多。在这些实验中,我们使用雄性 Ts65Dn 小鼠与它们的非三体雄性 2N 同窝仔鼠相比,通过电生理学详细研究了海马体 CA1 区的活动。我们发现 Ts65Dn 动物的 CA1 区位置细胞的空间特性正常。然而,我们发现,这些小鼠中海马体 CA1 位置细胞和γ节律与θ节律的相位关系发生了深刻改变。由于位置细胞活动和γ振荡在θ波上的相位组织被认为在海马体功能中起着关键作用,我们观察到的变化与最近的发现一致,即海马体网络的组织对于其功能比位置细胞的空间特性更为重要。最近的证据打破了空间缺陷与位置细胞异常相关的观点。在这些实验中,我们记录了唐氏综合征 Ts65Dn 小鼠模型的海马体位置细胞和局部场电位,发现位置细胞表现出表型正常,但位置细胞和γ节律与θ节律的关联发生了深刻变化,这表明整体网络状态对海马体功能至关重要。这些发现也与过量抑制控制是唐氏综合征海马体功能障碍的原因的证据一致。这些发现还证实了治疗唐氏综合征的新药物治疗途径。
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