Previous studies of Aβ plasma as a biomarker for Alzheimer's disease (AD) obtained conflicting results. We here included 715 subjects with baseline Aβ(1-40) and Aβ(1-42) plasma measurement (50% with 4 serial annual measurements): 205 cognitively normal controls (CN), 348 patients mild cognitive impairment (MCI) and 162 with AD. We assessed the factors that modified their concentrations and correlated these values with PIB PET, MRI and tau and Aβ(1-42) measures in cerebrospinal fluid (CSF). Association between Aβ and diagnosis (baseline and prospective) was assessed. A number of health conditions were associated with altered concentrations of plasma Aβ. The effect of age differed according to AD stage. Plasma Aβ(1-42) showed mild correlation with other biomarkers of Aβ pathology and were associated with infarctions in MRI. Longitudinal measurements of Aβ(1-40) and Aβ(1-42) plasma levels showed modest value as a prognostic factor for clinical progression. Our longitudinal study of complementary measures of Aβ pathology (PIB, CSF and plasma Aβ) and other biomarkers in a cohort with an extensive neuropsychological battery is significant because it shows that plasma Aβ measurements have limited value for disease classification and modest value as prognostic factors over the 3-year follow-up. However, with longer follow-up, within subject plasma Aβ measurements could be used as a simple and minimally invasive screen to identify those at increased risk for AD. Our study emphasizes the need for a better understanding of the biology and dynamics of plasma Aβ as well as the need for longer term studies to determine the clinical utility of measuring plasma Aβ.

译文

先前关于a β 血浆作为阿尔茨海默病 (AD) 生物标志物的研究获得了相互矛盾的结果。我们在这里包括715位具有基线a β(1-40) 和a β(1-42) 血浆测量 (50% 4个连续年度测量) 的受试者: 205位认知正常对照 (CN),348位轻度认知障碍 (MCI) 患者和AD 162。我们评估了改变其浓度的因素,并将这些值与脑脊液 (CSF) 中的PIB PET,MRI和tau和a β(1-42) 测量值相关联。评估a β 与诊断 (基线和前瞻性) 之间的相关性。许多健康状况与血浆A β 浓度的改变有关。年龄的影响因广告阶段而异。血浆a β(1-42) 与其他a β 病理生物标志物呈轻度相关性,并与MRI梗死相关。a β(1-40) 和a β(1-42) 血浆水平的纵向测量显示,作为临床进展的预后因素的价值不大。我们对具有广泛神经心理学电池的队列中a β 病理学 (PIB,CSF和血浆a β) 和其他生物标志物的补充措施的纵向研究具有重要意义,因为它表明血浆a β 测量对疾病分类的价值有限,并且作为预后因素的价值适中在3年的随访中。但是,随着随访时间的延长,受试者血浆a β 测量可以用作简单且微创的筛查,以识别那些AD风险增加的人。我们的研究强调需要更好地了解血浆a β 的生物学和动力学,以及需要进行长期研究以确定测量血浆a β 的临床用途。

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