摘要
背景:越来越多的证据强调神经炎症和趋化因子参与认知障碍病理生理学的关键作用。Fractalkine (CX3CL1)似乎是痴呆症发展的相关诱因,特别是在疾病的早期阶段。然而,有关脑脊液(CSF)和血液中CX3CL1水平的数据有限。此外,迄今为止,它作为MCI或AD的生物标志物的用途尚未被研究。 目的:本研究的目的是评估CX3CL1在早期诊断认知功能障碍中的临床应用。我们还比较了CX3CL1与其他与神经炎症相关的生物标志物的诊断价值。 方法:本研究共纳入认知障碍患者60例,其中AD患者42例,MCI患者18例,认知健康对照组20例。ELISA法检测脑脊液中CX3CL1、CCL-2、YKL-40的血药浓度和脑脊液中CX3CL1、CCL-2、YKL-40的血药浓度。 结果:与无认知障碍的老年人相比,MCI和AD患者的脑脊液和血液中CX3CL1浓度明显更高。非痴呆患者CX3CL1和YKL-40水平的升高与MCI相关。MCI受试者中CX3CL1的ROC曲线下面积比经典AD标记更大。 结论:目前的研究结果表明CX3CL1在认知障碍的病理过程中起着至关重要的作用,并且该蛋白在MCI和AD的早期诊断中具有潜在的价值。
关键词: 阿尔茨海默病,轻度认知障碍,CX3CL1
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