转录组分析揭示了阿尔茨海默病中海马的性别特异性模式。
Transcriptomic analysis reveals sex-specific patterns in the hippocampus in Alzheimer's disease.
机构信息
Translational Neuropharmacology Laboratory, Department of Psychology, University of Cyprus, Nicosia, Cyprus.
Neuroepidemiology Department, The Cyprus Institute of Neurology and Genetics, Nicosia, Cyprus.
出版信息
Front Endocrinol (Lausanne). 2024 Apr 16;15:1345498. doi: 10.3389/fendo.2024.1345498. eCollection 2024.
BACKGROUND
The hippocampus, vital for memory and learning, is among the first brain regions affected in Alzheimer's Disease (AD) and exhibits adult neurogenesis. Women face twice the risk of developing AD compare to men, making it crucial to understand sex differences in hippocampal function for comprehending AD susceptibility.
METHODS
We conducted a comprehensive analysis of bulk mRNA postmortem samples from the whole hippocampus (GSE48350, GSE5281) and its CA1 and CA3 subfields (GSE29378). Our aim was to perform a comparative molecular signatures analysis, investigating sex-specific differences and similarities in the hippocampus and its subfields in AD. This involved comparing the gene expression profiles among: (a) male controls (M-controls) vs. female controls (F-controls), (b) females with AD (F-AD) vs. F-controls, (c) males with AD (M-AD) vs. M-controls, and (d) M-AD vs. F-AD. Furthermore, we identified AD susceptibility genes interacting with key targets of menopause hormone replacement drugs, specifically the and genes, along with .
RESULTS
The hippocampal analysis revealed contrasting patterns between M-AD vs. M-controls and F-AD vs. F-controls, as well as M-controls vs. F-controls. Notably, , a key enzyme linked to amyloid-beta production in AD pathology, was found to be upregulated in M-controls compared to F-controls in both CA1 and CA3 hippocampal subfields. In M-AD vs. M-controls, the GABAergic synapse was downregulated, and the Estrogen signaling pathway was upregulated in both subfields, unlike in F-AD vs. F-controls. Analysis of the whole hippocampus also revealed upregulation of the GABAergic synapse in F-AD vs. F-controls. While direct comparison of M-AD vs. F-AD, revealed a small upregulation of the gene in the CA1 subfield of males. Conversely, F-AD vs. F-controls exhibited downregulation of the Dopaminergic synapse in both subfields, while the Calcium signaling pathway showed mixed regulation, being upregulated in CA1 but downregulated in CA3, unlike in M-AD vs. M-controls. The upregulated Estrogen signaling pathway in M-AD, suggests a compensatory response to neurodegenerative specifically in males with AD. Our results also identified potential susceptibility genes interacting with and , including and .
CONCLUSION
These findings underscore the importance of sex-specific disease mechanisms in AD pathogenesis. Region-specific analysis offers a more detailed examination of localized changes in the hippocampus, enabling to capture sex-specific molecular patterns in AD susceptibility and progression.
背景
海马体对记忆和学习至关重要,是阿尔茨海默病(AD)最先受到影响的大脑区域之一,并且存在成人神经发生。女性患 AD 的风险是男性的两倍,因此了解海马体功能的性别差异对于理解 AD 的易感性至关重要。
方法
我们对整个海马体(GSE48350,GSE5281)及其 CA1 和 CA3 亚区(GSE29378)的批量 mRNA 死后样本进行了全面分析。我们的目的是进行比较分子特征分析,研究 AD 中海马体及其亚区的性别特异性差异和相似性。这涉及到以下比较:(a)男性对照组(M-controls)与女性对照组(F-controls),(b)女性 AD 患者(F-AD)与 F-controls,(c)男性 AD 患者(M-AD)与 M-controls,以及(d)M-AD 与 F-AD。此外,我们鉴定了与绝经后激素替代药物的关键靶点相互作用的 AD 易感性基因,特别是 和 基因,以及 。
结果
海马体分析揭示了 M-AD 与 M-controls 和 F-AD 与 F-controls 之间以及 M-controls 与 F-controls 之间的对比模式。特别是,AD 病理中与淀粉样蛋白-β产生相关的关键酶 在 CA1 和 CA3 海马亚区中在 M-controls 中与 F-controls 相比上调。在 M-AD 与 M-controls 相比,GABA 能突触下调,而雌激素信号通路上调,而在 F-AD 与 F-controls 相比则不然。全海马体分析还揭示了 F-AD 与 F-controls 相比,GABA 能突触上调。而 M-AD 与 F-AD 的直接比较显示,男性 CA1 亚区 基因上调。相反,F-AD 与 F-controls 相比,两个亚区的多巴胺能突触下调,而钙信号通路表现出混合调节,CA1 上调,CA3 下调,而与 M-AD 与 M-controls 不同。M-AD 中上调的雌激素信号通路表明,特别是在男性 AD 中存在神经退行性变的代偿反应。我们的结果还确定了与 和 相互作用的潜在易感性基因,包括 和 。
结论
这些发现强调了 AD 发病机制中性别特异性疾病机制的重要性。区域特异性分析提供了对海马体局部变化的更详细检查,能够捕获 AD 易感性和进展中的性别特异性分子模式。
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