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两个独立研究队列中高危人群及阿尔茨海默病患者线粒体游离肉碱水平的性别差异

Sex differences in mitochondrial free-carnitine levels in subjects at-risk and with Alzheimer's disease in two independent study cohorts.

作者信息

Bigio Benedetta, Lima-Filho Ricardo A S, Barnhill Olivia, Sudo Felipe K, Drummond Claudia, Assunção Naima, Vanderborght Bart, Beasley James, Young Sarah, Korman Aryeh, Jones Drew R, Sultzer David L, Ferreira Sergio T, Mattos Paulo, Head Elizabeth, Tovar-Moll Fernanda, De Felice Fernanda G, Lourenco Mychael V, Nasca Carla

机构信息

Department of Psychiatry, New York University Grossman School of Medicine, New York, NY, USA.

Center for Dementia Research, Nathan S. Kline Institute for Psychiatric Research, Orangeburg, USA.

出版信息

Mol Psychiatry. 2025 Jun;30(6):2573-2583. doi: 10.1038/s41380-024-02862-5. Epub 2025 Jan 7.

Abstract

A major challenge in the development of more effective therapeutic strategies for Alzheimer's disease (AD) is the identification of molecular mechanisms linked to specific pathophysiological features of the disease. Importantly AD has a two-fold higher incidence in women than men and a protracted prodromal phase characterized by amnestic mild-cognitive impairment (aMCI) suggesting that biological processes occurring early can initiate vulnerability to AD. Here, we used a sample of 125 subjects from two independent study cohorts to determine the levels in plasma (the most accessible specimen) of two essential mitochondrial markers acetyl-L-carnitine (LAC) and its derivative free-carnitine motivated by a mechanistic model in rodents in which targeting mitochondrial metabolism of LAC leads to the amelioration of cognitive function and boosts epigenetic mechanisms of gene expression. We report a sex-specific deficiency in free-carnitine levels in women with aMCI and early-AD compared to cognitively healthy controls; no change was observed in men. We also replicated the prior finding of decreased LAC levels in both women and men with AD, supporting the robustness of the study samples assayed in our new study. The magnitude of the sex-specific free-carnitine deficiency reflected the severity of cognitive dysfunction and held in two study cohorts. Furthermore, patients with the lower free-carnitine levels showed higher β-amyloid(Aβ) accumulation and t-Tau levels assayed in cerebrospinal fluid (CSF). Computational analyses showed that the mitochondrial markers assayed in plasma are at least as accurate as CSF measures to classify disease status. Together with the mechanistic platform in rodents, these translational findings lay the groundwork to create preventive individualized treatments targeting sex-specific changes in mitochondrial metabolism that may be subtle to early cognitive dysfunction of AD risk.

摘要

开发更有效的阿尔茨海默病(AD)治疗策略面临的一个主要挑战是确定与该疾病特定病理生理特征相关的分子机制。重要的是,AD在女性中的发病率比男性高两倍,且有一个以遗忘型轻度认知障碍(aMCI)为特征的漫长前驱期,这表明早期发生的生物学过程可引发对AD的易感性。在此,我们使用来自两个独立研究队列的125名受试者样本,根据啮齿动物的一个机制模型,来测定血浆(最易获取的样本)中两种重要线粒体标志物乙酰-L-肉碱(LAC)及其衍生物游离肉碱的水平,在该模型中,靶向LAC的线粒体代谢可改善认知功能并促进基因表达的表观遗传机制。我们报告,与认知健康的对照组相比,患有aMCI和早期AD的女性游离肉碱水平存在性别特异性缺乏;男性未观察到变化。我们还重复了之前关于AD女性和男性LAC水平降低的发现,支持了我们新研究中所检测研究样本的可靠性。性别特异性游离肉碱缺乏的程度反映了认知功能障碍的严重程度,且在两个研究队列中均成立。此外,游离肉碱水平较低的患者脑脊液(CSF)中检测到的β-淀粉样蛋白(Aβ)积累和总tau蛋白(t-Tau)水平较高。计算分析表明,血浆中检测的线粒体标志物在分类疾病状态方面至少与CSF测量一样准确。结合啮齿动物的机制平台,这些转化研究结果为制定预防性个体化治疗奠定了基础,该治疗针对线粒体代谢中的性别特异性变化,这些变化可能对AD风险的早期认知功能障碍较为微妙。

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