阿尔茨海默氏症模型小鼠海马不成熟、pH 值降低和神经过度兴奋的基因表达特征

IF 2 Q3 NEUROSCIENCES

Neuropsychopharmacology Reports Pub Date : 2025-03-01 DOI:10.1002/npr2.70001

Sayaka Naganishi, Hideo Hagihara, Tsuyoshi Miyakawa

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引用次数: 0

摘要

目的：阿尔茨海默病（AD）是痴呆症的主要原因，患病率越来越高。MAPT、PSEN1和PSEN2等基因的突变是导致几种AD模型小鼠发展的危险因素。最近的假设表明，AD的脑部病理包括神经发育异常、pH值降低和神经过度兴奋。然而，目前尚不清楚这些病理在多大程度上反映在AD模型的基因表达变化中。本研究旨在比较多种AD模型小鼠大脑中与这三个因素相关的基因表达模式，评估重叠程度。方法：全面检索公共数据库，收集20个AD模型小鼠海马基因表达数据集。将这些数据集与海马成熟、脑pH值和神经过度兴奋相关的基因集进行比较，以统计评估重叠。途径富集分析探讨了这些基因表达变化的生物学相关性。结果：在不同的AD模型中，与成熟度、pH值和过度兴奋相关基因的重叠程度各不相同，表明成熟度较低、pH值较低和神经过度兴奋增加之间存在显著相关性。在MAPT突变体和APP+PSEN1纯合转基因小鼠中，随着年龄的增长，这些特征变得更加明显。通路荟萃分析显示，AD模型中与成熟度、pH值和过度兴奋相关的基因参与突触和通道功能以及炎症反应，与先前的研究一致。结论：这些研究结果表明，与成熟度、pH值和神经过度兴奋相关的病理生理变化在个体AD模型小鼠中起不同的作用。我们最近的研究发现，人类AD患者的疾病进展与实际pH值呈负相关。考虑到本研究的结果，与pH值相关的成熟度和神经过度兴奋也可能与疾病进展有关。因此，这些因素的基因表达变化可能是评估AD模型病理的有用标记。

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Gene Expression Signatures of Immaturity, Decreased pH, and Neural Hyperexcitation in the Hippocampus of Alzheimer's Disease Model Mice.

Aims: Alzheimer's disease (AD) is a leading cause of dementia, with increasing prevalence. Mutations in genes like MAPT, PSEN1, and PSEN2 are risk factors, leading to the development of several AD model mice. Recent hypotheses suggest AD brain pathology involves abnormal neurodevelopment, decreased pH, and neural hyperexcitation. However, it remains unclear to what extent these pathologies are reflected in the gene expression changes of AD models. This study aims to compare gene expression patterns in the brains of multiple AD model mice with those related to these three factors, evaluating the extent of overlap.

Methods: We conducted a comprehensive search of public databases, collecting 20 gene expression datasets from the hippocampus of AD model mice. These datasets were compared with gene sets related to hippocampal maturation, brain pH, and neural hyperexcitation to statistically assess overlap. Pathway enrichment analysis explored the biological relevance of these gene expression changes.

Results: The extent of overlap with maturity-, pH-, and hyperexcitation-associated genes varied across AD models, showing significant correlations between lower maturity, lower pH, and increased neural hyperexcitation. In MAPT mutant and APP+PSEN1 homozygous transgenic mice, these signatures became more pronounced with age. Pathway meta-analysis revealed that genes associated with maturity, pH, and hyperexcitation in AD models are involved in synaptic and channel functions, as well as inflammatory responses, consistent with previous studies.

Conclusion: These findings suggest that pathophysiological changes related to maturity, pH, and neural hyperexcitation play varying roles across individual AD model mice. Our recent study found a negative correlation between disease progression and actual pH levels in human AD patients. Considering the results presented in this study, maturity and neural hyperexcitation, which are correlated with pH, may also be linked to disease progression. Thus, gene expression changes in these factors could be useful markers for assessing the pathology in AD models.

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来源期刊

Neuropsychopharmacology Reports Psychology-Clinical Psychology

CiteScore

3.60

自引率

4.00%

发文量

审稿时长

14 weeks