酒精使用障碍中的血浆载脂蛋白和记忆功能：在雄性C57BL/6J小鼠和男性中的发现提示APOAI的作用

IF 2.7 Q2 SUBSTANCE ABUSE

Alcohol (Hanover, York County, Pa.) Pub Date : 2025-08-22 DOI:10.1111/acer.70149

Berta Escudero, Max Kreifeldt, Kiera Fleck, Catherine Lopez, Candice Contet, Laura Orio

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引用次数: 0

摘要

背景：记忆障碍在酒精使用障碍（AUD）患者中很常见，我们缺乏特异性的生物标志物来检测它。某些载脂蛋白与认知有关，携带APOE4基因是AUD患者记忆障碍的易感因素。我们研究了酒精依赖雄性小鼠和人类与对照组相比的记忆缺陷，以及它们与载脂蛋白AI （APOAI）、载脂蛋白B （APOB）和载脂蛋白E （APOE）血浆水平的关系。方法：雄性C57BL/6J小鼠自愿饮酒（两瓶选择，2BC）和慢性间歇乙醇蒸气暴露（CIE）作为酒精依赖模型；采用目标定位测试（OLT）和新目标识别测试（NORT）评估记忆。此外，在西班牙酒精失调项目中招募了男性aud诊断患者，并通过韦氏记忆量表iv （WMS-IV）进行评估。采用ELISA试剂盒和Luminex免疫测定技术检测小鼠和人血浆APOAI、APOB和APOE水平。在小鼠早期戒酒和饮酒后的大脑中定量测定APOAI免疫标记。结果：与Air-2BC对照组（n = 11）相比，CIE-2BC小鼠（n = 8）饮酒增加，并表现出空间记忆（OLT）和识别记忆（NORT）的缺陷，而AUD患者（n = 12）与对照组（n = 16）相比，表现出语言和视觉记忆（WMS-IV）的缺陷。在CIE-2BC小鼠和AUD患者中检测到较高的APOAI血浆水平，动物和人的APOB和APOE无差异。在整个样本中，APOAI、APOB和APOE水平与记忆功能测试/量表之间存在显著的负相关，APOAI在动物和人类中都显示出一致的结果。在小鼠皮层下器官检测到APOAI免疫反应性，但在实验组之间没有差异。结论：CIE-2BC小鼠和AUD患者在早期戒断期间均表现出血浆APOAI水平升高。在这两个物种中，APOAI与较差的记忆表现相关，这表明这种载脂蛋白在酒精诱导的认知障碍中可能起作用。

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Plasma apolipoproteins and memory function in alcohol use disorder: Findings in male C57BL/6J mice and men suggest a role for APOAI.

Background: Memory impairment is frequent among alcohol use disorder (AUD) patients, and we lack specific biomarkers to detect it. Certain apolipoproteins were linked to cognition, and carrying the APOE4 gene is a vulnerability factor to memory impairment in AUD patients. We explored memory deficits in alcohol-dependent male mice and humans versus controls, and their relationship to Apolipoprotein AI (APOAI), apolipoprotein B (APOB), and apolipoprotein E (APOE) plasma levels.

Methods: Male C57BL/6J mice underwent voluntary alcohol drinking (two-bottle choice, 2BC) and chronic intermittent ethanol vapor exposure (CIE) as a model of alcohol dependence; memory was assessed by the Object Location Test (OLT) and Novel Object Recognition Test (NORT). Additionally, male AUD-diagnosed patients were recruited in Spain during an alcohol dishabituation program and assessed by the Wechsler Memory Scale-IV (WMS-IV). Plasma APOAI, APOB, and APOE levels were checked in mice and humans by ELISA kits and Luminex immunoassay technology. APOAI immunolabeling was quantified in mouse brain in early withdrawal and following alcohol consumption.

Results: CIE-2BC mice (n = 8) escalated alcohol consumption compared to Air-2BC controls (n = 11) and showed deficits in spatial memory (OLT) and recognition memory (NORT) while AUD patients (n = 12) showed deficits in verbal and visual memory (WMS-IV) versus controls (n = 16). Higher plasma levels of APOAI were detected in CIE-2BC mice and AUD patients, with no differences in APOB and APOE in animals and humans. Significant negative correlations were found between levels of APOAI, APOB, and APOE and memory function tests/scales in the entire sample, with APOAI showing consistent results in both animals and humans. APOAI immunoreactivity was detected in the mice subfornical organ, but the signal did not differ between experimental groups.

Conclusions: Both CIE-2BC mice and AUD patients exhibited elevated plasma levels of APOAI during early abstinence. APOAI correlated with poorer memory performance in both species, suggesting a potential role for this apolipoprotein in the context of alcohol-induced cognitive impairment.

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来源期刊

Alcohol (Hanover, York County, Pa.)

CiteScore

5.40

自引率

0.00%

发文量