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在阿尔茨海默病的Tg2576模型中,齿状回苔藓细胞的兴奋性增加在生命早期就会出现。

Increased excitability of dentate gyrus mossy cells occurs early in life in the Tg2576 model of Alzheimer's disease.

作者信息

Alcantara-Gonzalez David, Kennedy Meghan, Criscuolo Chiara, Botterill Justin, Scharfman Helen E

机构信息

Center for Dementia Research, The Nathan Kline Institute for Psychiatric Research, 140 Old Orangeburg Rd. Bldg. 39, Orangeburg, NY, 10962, USA.

Department of Child & Adolescent Psychiatry, Neuroscience & Physiology, and Psychiatry, New York University Langone Health, New York City, NY, 10016, USA.

出版信息

Alzheimers Res Ther. 2025 May 15;17(1):105. doi: 10.1186/s13195-025-01747-1.

Abstract

BACKGROUND

Hyperexcitability in Alzheimer's disease (AD) is proposed to emerge early and contribute to disease progression. The dentate gyrus (DG) and its primary cell type, granule cells (GCs) are implicated in hyperexcitability in AD. Hence, we hypothesized that mossy cells (MCs), important regulators of GC excitability, contribute to early hyperexcitability in AD. Indeed, MCs and GCs are linked to hyperexcitability in epilepsy.

METHODS

Using the Tg2576 model of AD and WT mice (~ 1 month-old), we compared MCs and GCs electrophysiologically and morphologically, assessed the activity marker c-Fos, Aβ expression and a hippocampal- and MC-dependent memory task that is impaired at 3-4 months of age in Tg2576 mice.

RESULTS

Tg2576 MCs had increased spontaneous excitatory events (sEPSP/Cs) and decreased spontaneous inhibitory currents (sIPSCs), increasing the excitation/inhibition ratio. Additionally, Tg2576 MC intrinsic excitability was enhanced. Consistent with in vitro results, Tg2576 MCs showed enhanced c-Fos protein expression. Tg2576 MCs had increased intracellular Aβ expression, suggesting a reason for increased excitability. GCs showed increased excitatory and inhibitory input without changes in intrinsic properties, consistent with effects of increased MC activity. In support, increased GC activity was normalized by an antagonist of MC input to GCs. Also in support, Tg2576 MC axons showed sprouting to the area of GC dendrites. These effects occurred before an impairment in the memory task, suggesting they are extremely early alterations.

CONCLUSIONS

Alterations in Tg2576 MCs and GCs early in life suggest an early role for MCs in increased GC excitability. MCs may be a novel target to intervene in AD pathophysiology at early stages.

摘要

背景

阿尔茨海默病(AD)中的过度兴奋性被认为在疾病早期出现并促进疾病进展。齿状回(DG)及其主要细胞类型颗粒细胞(GCs)与AD中的过度兴奋性有关。因此,我们假设苔藓细胞(MCs)作为GCs兴奋性的重要调节因子,促成了AD早期的过度兴奋性。事实上,MCs和GCs与癫痫中的过度兴奋性有关。

方法

使用AD的Tg2576模型和野生型小鼠(约1月龄),我们在电生理学和形态学上比较了MCs和GCs,评估了活性标记物c-Fos、Aβ表达以及一项海马和MC依赖的记忆任务,该任务在Tg2576小鼠3至4月龄时受损。

结果

Tg2576 MCs的自发兴奋性事件(sEPSP/Cs)增加,自发抑制性电流(sIPSCs)减少,从而增加了兴奋/抑制比。此外,Tg2576 MCs的内在兴奋性增强。与体外结果一致,Tg2576 MCs显示c-Fos蛋白表达增强。Tg2576 MCs的细胞内Aβ表达增加,提示兴奋性增加的原因。GCs的兴奋性和抑制性输入增加,但其内在特性没有变化,这与MC活性增加的影响一致。作为支持,通过GCs的MC输入拮抗剂可使GC活性增加恢复正常。同样作为支持,Tg2576 MC轴突向GC树突区域发芽。这些效应发生在记忆任务受损之前,表明它们是非常早期的改变。

结论

生命早期Tg2576 MCs和GCs的改变表明MCs在增加GC兴奋性方面起早期作用。MCs可能是早期干预AD病理生理学的新靶点。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/332e/12079945/94110a1d2450/13195_2025_1747_Fig1_HTML.jpg

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