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Neuropsychological Criteria for Mild Cognitive Impairment Improves Diagnostic Precision Biomarker Associations and Progression Rates

机译:轻度认知障碍的神经心理学标准可提高诊断准确性生物标志物关联性和进展率

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摘要

We compared two methods of diagnosing mild cognitive impairment (MCI): conventional Petersen/Winblad criteria as operationalized by the Alzheimer’s Disease Neuroimaging Initiative (ADNI) and an actuarial neuropsychological method put forward by Jak and Bondi designed to balance sensitivity and reliability. 1,150 ADNI participants were diagnosed at baseline as cognitively normal (CN) or MCI via ADNI criteria (MCI: n = 846; CN: n = 304) or Jak/Bondi criteria (MCI: n = 401; CN: n = 749), and the two MCI samples were submitted to cluster and discriminant function analyses. Resulting cluster groups were then compared and further examined for APOE allelic frequencies, cerebrospinal fluid (CSF) Alzheimer’s disease (AD) biomarker levels, and clinical outcomes. Results revealed that both criteria produced a mildly impaired Amnestic subtype and a more severely impaired Dysexecutive/Mixed subtype. The neuropsychological Jak/Bondi criteria uniquely yielded a third Impaired Language subtype, whereas conventional Petersen/Winblad ADNI criteria produced a third subtype comprising nearly one-third of the sample that performed within normal limits across the cognitive measures, suggesting this method’s susceptibility to false positive diagnoses. MCI participants diagnosed via neuropsychological criteria yielded dissociable cognitive phenotypes, significant CSF AD biomarker associations, more stable diagnoses, and identified greater percentages of participants who progressed to dementia than conventional MCI diagnostic criteria. Importantly, the actuarial neuropsychological method did not produce a subtype that performed within normal limits on the cognitive testing, unlike the conventional diagnostic method. Findings support the need for refinement of MCI diagnoses to incorporate more comprehensive neuropsychological methods, with resulting gains in empirical characterization of specific cognitive phenotypes, biomarker associations, stability of diagnoses, and prediction of progression. Refinement of MCI diagnostic methods may also yield gains in biomarker and clinical trial study findings because of improvements in sample compositions of ‘true positive’ cases and removal of ‘false positive’ cases.
机译:我们比较了两种诊断轻度认知障碍(MCI)的方法:由阿尔茨海默氏病神经影像学倡议(ADNI)实施的常规Petersen / Winblad标准和由Jak和Bondi提出的旨在平衡敏感性和可靠性的精算神经心理学方法。通过ADNI标准(MCI:n = 846; CN:n = 304)或Jak / Bondi标准(MCI:n = 401; CN:n = 749)在基线将1,150名ADNI参与者诊断为认知正常(CN)或MCI,并将这两个MCI样本提交给聚类和判别函数分析。然后比较结果的群集组,并进一步检查其APOE等位基因频率,脑脊液(CSF)阿尔茨海默氏病(AD)生物标志物水平和临床结果。结果显示,这两个标准均产生轻度受损的记忆删除亚型和严重受损的Dysexecutive / Mixed亚型。神经心理学的Jak / Bondi标准唯一地产生了第三种障碍语言亚型,而常规的Petersen / Winblad ADNI标准则产生了第三种亚型,包括在整个认知测量范围内均在正常范围内进行的样本的近三分之一,表明该方法对假阳性的敏感性。诊断。通过神经心理学标准诊断的MCI参与者产生了可分离的认知表型,显着的CSF AD生物标志物关联,更稳定的诊断,并且与常规MCI诊断标准相比,进展为痴呆的参与者所占的百分比更高。重要的是,与传统的诊断方法不同,精算神经心理学方法不会产生在认知测试的正常范围内执行的亚型。研究结果支持对MCI诊断进行细化以纳入更全面的神经心理学方法的需求,从而在特定认知表型,生物标记关联,诊断的稳定性和进展的预测的经验表征方面获得了进步。由于“真阳性”病例的样本组成有所改善,而“假阳性”病例的去除也有所改善,因此改进MCI诊断方法也可能会在生物标志物和临床试验研究结果中带来收益。

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