APOE ε4携带与海马-嗅道功能连通性相关

Toshikazu Ikuta, Taylor Bither
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引用次数: 0

摘要

嗅觉功能障碍通常出现在认知症状之前,可能预示着神经退行性过程的早期易感性。本研究考察了遗传风险,特别是载脂蛋白E中epsilon 4等位基因的存在,是否与海马体和嗅觉相关大脑区域之间功能连接的改变有关。126名参与者静息状态功能成像数据(平均年龄71.8岁,SD = 6.9;67名女性)在一系列临床阶段进行了分析。计算海马与四个嗅觉相关区域之间的功能连通性:前梨状皮质、后梨状皮质、嗅球和嗅束。多元回归模型评估遗传风险、年龄、性别和临床诊断是否预测连接强度。遗传风险与海马与嗅球和嗅道之间的连通性增加显著相关,而在梨状皮质区域没有观察到显著影响。临床诊断不是任何地区连通性的显著预测因子。这些结果表明,遗传风险与特定嗅觉-海马通路的早期功能重组有关,特别是嗅觉道,与临床疾病阶段无关。嗅觉-海马体网络可能是检测与神经退行性风险相关的早期大脑变化的敏感靶点。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
APOE ε4 Carriage is Associated with Hippocampus-Olfactory Tract Functional Connectivity.

Olfactory dysfunction often emerges before cognitive symptoms and may signal early vulnerability to neurodegenerative processes. This study examined whether genetic risk, specifically the presence of the epsilon 4 allele in apolipoprotein E, is associated with altered functional connectivity between the hippocampus and olfactory-related brain regions. Resting-state functional imaging data from 126 participants (mean age = 71.8 years, SD = 6.9; 67 females) across a range of clinical stages were analyzed. Functional connectivity was computed between the hippocampus and four olfactory-related regions: anterior piriform cortex, posterior piriform cortex, olfactory bulb, and olfactory tract. Multiple regression models assessed whether genetic risk, age, sex, and clinical diagnosis predicted connectivity strength. Genetic risk was significantly associated with increased connectivity between the hippocampus and both the olfactory bulb and olfactory tract, while no significant effects were observed in the piriform cortex regions. Clinical diagnosis was not a significant predictor of connectivity in any region. These results suggest that genetic risk is linked to early functional reorganization in specific olfactory-hippocampal pathways, particularly the olfactory tract, independent of clinical disease stage. The olfactory-hippocampal network may serve as a sensitive target for detecting early brain changes associated with neurodegenerative risk.

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