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A multicentre longitudinal study of flortaucipir (18F) in normal ageing, mild cognitive impairment and Alzheimer's disease dementia.多中心纵向研究氟替卡滨(18F)在正常衰老、轻度认知障碍和阿尔茨海默病痴呆中的作用。
Brain. 2019 Jun 1;142(6):1723-1735. doi: 10.1093/brain/awz090.
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ATN profiles among cognitively normal individuals and longitudinal cognitive outcomes.认知正常个体的 ATN 特征与纵向认知结局。
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Alzheimers Dement (Amst). 2018 Apr 21;10:346-357. doi: 10.1016/j.dadm.2018.03.004. eCollection 2018.
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The development and validation of tau PET tracers: current status and future directions.tau蛋白正电子发射断层显像剂的研发与验证:现状与未来方向
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NIA-AA Research Framework: Toward a biological definition of Alzheimer's disease.NIA-AA 研究框架:迈向阿尔茨海默病的生物学定义。
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使用脑脊液磷酸化tau 和 AV1451 正电子发射断层扫描技术对阿尔茨海默病生物标志物差异进行特征分析。

Characterization of Alzheimer Disease Biomarker Discrepancies Using Cerebrospinal Fluid Phosphorylated Tau and AV1451 Positron Emission Tomography.

机构信息

Douglas Mental Health University Institute, Studies on Prevention of Alzheimer's Disease Centre, Montreal, Quebec, Canada.

Department of Psychiatry, McGill University, Montreal, Quebec, Canada.

出版信息

JAMA Neurol. 2020 Apr 1;77(4):508-516. doi: 10.1001/jamaneurol.2019.4749.

DOI:10.1001/jamaneurol.2019.4749
PMID:31961372
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC6990861/
Abstract

IMPORTANCE

Fluid and imaging biomarkers of Alzheimer disease (AD) are often used interchangeably, but some biomarkers may reveal earlier stages of disease.

OBJECTIVE

To characterize individuals with tau abnormality indicated by cerebrospinal fluid (CSF) assay or positron emission tomography (PET).

DESIGN, SETTING, AND PARTICIPANTS: Between 2010 and 2019, 322 participants in the Alzheimer's Disease Neuroimaging Initiative (ADNI) underwent CSF and PET assessments of tau pathology. Data-driven, clinically relevant thresholds for CSF phosphorylated tau (P-tau) (≥26.64 pg/mL) and flortaucipir-PET meta-regions of interest (ROI) (standard uptake value ratio ≥1.37) indicated participants' tau status as CSF-/PET-, CSF+/PET-, CSF-/PET+, and CSF+/PET+. Of 1659 ADNI participants with a CSF or flortaucipir assessment, 588 had both measures (1071 were excluded). Among these, 266 were further excluded because they did not have flortaucipir and CSF testing within less than 25 months, leaving 322 for analysis. Of these, 213 were cognitively unimpaired (CU); 98 had mild cognitive impairment (MCI); and 11 had AD dementia.

MAIN OUTCOMES AND MEASURES

We compared tau-positive vs tau-negative groups as indicated by either modality or demographic and clinical variables, amyloid β-PET burden, and flortaucipir-PET binding across Braak stage-related ROIs. We also compared 5-year rates of CSF P-tau accumulation and cognitive decline prior to flortaucipir-PET scanning.

RESULTS

Among the 322 study participants, 180 were women (56%), and the mean (SD) age was 73.08 (7.37) years. Two hundred ten participants were CSF-/PET- (65%); 63 were CSF+/PET- (19.5%); 15 were CSF-/PET+ (4.6%); and 34 were CSF+/PET+ (10.5%). Most CSF-/PET+ participants had measures near CSF or PET tau thresholds. The CSF+/PET- participants showed faster 5-year accrual of P-tau and increased flortaucipir-PET binding in early Braak ROIs but similar memory decline compared with CSF-/PET- participants. Tau-positive individuals by either measure showed increased amyloid β-PET burden. All CSF+/PET+ individuals were amyloid-positive, and 26 had MCI or AD dementia (76%). Compared with the CSF-/PET- group, CSF+/PET+ individuals had experienced faster 5-year accrual of CSF P-tau and decline in memory and executive function, resulting in reduced cognitive abilities at the time of flortaucipir-PET assessment.

CONCLUSIONS AND RELEVANCE

Suprathreshold CSF P-tau without flortaucipir-PET abnormality may indicate a stage of AD development characterized by early tau abnormality without measurable loss in cognitive performance. Persons with both tau CSF and PET abnormality appear to have reduced cognitive capacities resulting from faster antecedent cognitive decline. Elevation of CSF P-tau appears to precede flortaucipir-PET positivity in the progression of AD pathogenesis and related cognitive decline.

摘要

重要性

阿尔茨海默病(AD)的流体和成像生物标志物经常被互换使用,但有些生物标志物可能揭示出疾病的早期阶段。

目的

描述通过脑脊液(CSF)检测或正电子发射断层扫描(PET)显示 tau 异常的个体。

设计、地点和参与者:在 2010 年至 2019 年期间,ADNI 中的 322 名参与者接受了 CSF 和 tau 病理学 PET 评估。数据驱动的、临床相关的 CSF 磷酸化 tau(P-tau)(≥26.64pg/ml)和 flortaucipir-PET 感兴趣区(ROI)的阈值(标准摄取比值≥1.37)表明参与者的 tau 状态为 CSF-/PET-、CSF+/PET-、CSF-/PET+和 CSF+/PET+。在 1659 名接受 CSF 或 flortaucipir 评估的 ADNI 参与者中,有 588 名参与者同时进行了这两项检查(有 1071 名参与者被排除在外)。在这些参与者中,有 266 名由于在不到 25 个月内没有进行 flortaucipir 和 CSF 检查而被进一步排除,剩下 322 名用于分析。其中,213 名认知正常(CU);98 名患有轻度认知障碍(MCI);11 名患有 AD 痴呆。

主要结果和措施

我们比较了 tau 阳性和 tau 阴性组,这些组是根据任一模态或人口统计学和临床变量、淀粉样蛋白β-PET 负担以及与 Braak 阶段相关的 ROI 中的 flortaucipir-PET 结合来确定的。我们还比较了 CSF P-tau 积累和 flortaucipir-PET 扫描前认知下降的 5 年率。

结果

在 322 名研究参与者中,有 180 名女性(56%),平均(SD)年龄为 73.08(7.37)岁。210 名参与者为 CSF-/PET-(65%);63 名 CSF+/PET-(19.5%);15 名 CSF-/PET+(4.6%);34 名 CSF+/PET+(10.5%)。大多数 CSF-/PET+参与者的测量值接近 CSF 或 PET tau 阈值。CSF+/PET-参与者的 P-tau 在 5 年内的累积速度更快,并且在早期 Braak ROI 中 flortaucipir-PET 结合增加,但与 CSF-/PET-参与者相比,记忆下降相似。通过任何一种方法检测到 tau 阳性的个体都显示出淀粉样蛋白β-PET 负担增加。所有 CSF+/PET+个体均为淀粉样蛋白阳性,其中 26 名患有 MCI 或 AD 痴呆(76%)。与 CSF-/PET-组相比,CSF+/PET+个体的 CSF P-tau 在 5 年内的累积速度更快,记忆和执行功能下降,导致在 flortaucipir-PET 评估时认知能力下降。

结论和相关性

没有 flortaucipir-PET 异常的超阈值 CSF P-tau 可能表明 AD 发展的一个阶段,其特征是早期 tau 异常,而认知表现没有可测量的损失。同时存在 tau CSF 和 PET 异常的个体似乎由于认知能力下降更快而导致认知能力降低。CSF P-tau 的升高似乎先于 AD 发病机制和相关认知下降的 flortaucipir-PET 阳性。