Plasma Phosphorylated Tau 217 and Aβ42/40 to Predict Early Brain Aβ Accumulation in People Without Cognitive Impairment.

IF 20.4 1区 医学 Q1 CLINICAL NEUROLOGY JAMA neurology Pub Date : 2024-09-01 DOI:10.1001/jamaneurol.2024.2619
Shorena Janelidze, Nicolas R Barthélemy, Gemma Salvadó, Suzanne E Schindler, Sebastian Palmqvist, Niklas Mattsson-Carlgren, Joel B Braunstein, Vitaliy Ovod, James G Bollinger, Yingxin He, Yan Li, Cyrus A Raji, John C Morris, David M Holtzman, Nicholas J Ashton, Kaj Blennow, Erik Stomrud, Randall J Bateman, Oskar Hansson
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Abstract

Importance: Phase 3 trials of successful antiamyloid therapies in Alzheimer disease (AD) have demonstrated improved clinical efficacy in people with less severe disease. Plasma biomarkers will be essential for efficient screening of participants in future primary prevention clinical trials testing antiamyloid therapies in cognitively unimpaired (CU) individuals with initially low brain β-amyloid (Aβ) levels who are at high risk of accumulating Aβ.

Objective: To investigate if combining plasma biomarkers could be useful in predicting subsequent development of Aβ pathology in CU individuals with subthreshold brain Aβ levels (defined as Aβ levels <40 Centiloids) at baseline.

Design, setting, and participants: This was a longitudinal study including Swedish BioFINDER-2 (enrollment 2017-2022) and replication in 2 independent cohorts, the Knight Alzheimer Disease Research Center (Knight ADRC; enrollment 1988 and 2019) and Swedish BioFINDER-1 (enrollment 2009-2015). Included for analysis was a convenience sample of CU individuals with baseline plasma phosphorylated tau 217 (p-tau217) and Aβ42/40 assessments and Aβ assessments with positron emission tomography (Aβ-PET) or cerebrospinal fluid (CSF) Aβ42/40. Data were analyzed between April 2023 and May 2024.

Exposures: Baseline plasma levels of Aβ42/40, p-tau217, the ratio of p-tau217 to nonphosphorylated tau (%p-tau217), p-tau231, and glial fibrillary acidic protein (GFAP).

Main outcomes and measures: Cross-sectional and longitudinal PET and CSF measures of brain Aβ pathology.

Results: This study included 495 (BioFINDER-2), 283 (Knight ADRC), and 205 (BioFINDER-1) CU participants. In BioFINDER-2, the mean (SD) age was 65.7 (14.4) with 261 females (52.7%). When detecting abnormal CSF Aβ-status, a combination of plasma %p-tau217 and Aβ42/40 showed better performance (area under the curve = 0.949; 95% CI, 0.929-0.970; P <.02) than individual biomarkers. In CU participants with subthreshold baseline Aβ-PET, baseline plasma %p-tau217 and Aβ42/40 levels were significantly associated with baseline Aβ-PET (n = 384) and increases in Aβ-PET over time (n = 224). Associations of plasma %p-tau217 and Aβ42/40 and their interaction with baseline Aβ-PET (%p-tau217: β = 2.77; 95% CI, 1.84-3.70; Aβ42/40: β = -1.64; 95% CI, -2.53 to -0.75; %p-tau217 × Aβ42/40: β = -2.14; 95% CI, -2.79 to -1.49; P < .001) and longitudinal Aβ-PET (%p-tau217: β = 0.67; 95% CI, 0.48-0.87; Aβ42/40: β = -0.33; 95% CI, -0.51 to -0.15; %p-tau217 × Aβ42/40: β = -0.31; 95% CI, -0.44 to -0.18; P < .001) were also significant in the models combining the 2 baseline biomarkers as predictors. Similarly, baseline plasma p-tau217 and Aβ42/40 were independently associated with longitudinal Aβ-PET in Knight ADRC (%p-tau217: β = 0.71; 95% CI, 0.26-1.16; P = .002; Aβ42/40: β = -0.74; 95% CI, -1.26 to -0.22; P = .006) and longitudinal CSF Aβ42/40 in BioFINDER-1 (p-tau217: β = -0.0003; 95% CI, -0.0004 to -0.0001; P = .01; Aβ42/40: β = 0.0004; 95% CI, 0.0002-0.0006; P < .001) in CU participants with subthreshold Aβ levels at baseline. Plasma p-tau231 and GFAP did not provide any clear independent value.

Conclusions and relevance: Results of this cohort study suggest that combining plasma p-tau217and Aβ42/40 levels could be useful for predicting development of Aβ pathology in people with early stages of subthreshold Aβ accumulation. These biomarkers might thus facilitate screening of participants for future primary prevention trials.

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用血浆磷酸化 Tau 217 和 Aβ42/40 预测无认知障碍人群的早期脑 Aβ 累积。
重要性:成功治疗阿尔茨海默病(AD)的抗淀粉样蛋白疗法的第三阶段试验表明,病情较轻的患者的临床疗效有所改善。血浆生物标志物对于有效筛选未来初级预防临床试验的参与者至关重要,这些临床试验针对的是最初脑β淀粉样蛋白(Aβ)水平较低但Aβ累积风险较高的认知功能未受损(CU)个体的抗淀粉样蛋白疗法:研究结合血浆生物标志物是否有助于预测脑 Aβ 水平低于阈值(定义为 Aβ 水平)的 CU 患者 Aβ 病理学的后续发展:这是一项纵向研究,包括瑞典 BioFINDER-2(2017-2022 年入组)和两个独立队列(奈特阿尔茨海默病研究中心(Knight ADRC;1988 年和 2019 年入组)和瑞典 BioFINDER-1(2009-2015 年入组))的复制。纳入分析的是基线血浆磷酸化tau 217(p-tau217)和Aβ42/40评估以及正电子发射断层扫描(Aβ-PET)或脑脊液(CSF)Aβ42/40评估的CU个体方便样本。数据分析时间为 2023 年 4 月至 2024 年 5 月:Aβ42/40、p-tau217、p-tau217与非磷酸化tau的比率(%p-tau217)、p-tau231和胶质纤维酸性蛋白(GFAP)的血浆基线水平:主要结果和测量方法:横向和纵向PET和CSF脑Aβ病理学测量方法:这项研究包括 495 名(BioFINDER-2)、283 名(Knight ADRC)和 205 名(BioFINDER-1)中U 参与者。在 BioFINDER-2 中,平均(标清)年龄为 65.7(14.4)岁,女性 261 人(52.7%)。在检测异常 CSF Aβ 状态时,血浆 %p-tau217 和 Aβ42/40 的组合显示出更好的性能(曲线下面积 = 0.949;95% CI,0.929-0.970;P):这项队列研究的结果表明,结合血浆 p-tau217 和 Aβ42/40 水平可用于预测阈下 Aβ 累积早期患者 Aβ 病理学的发展。因此,这些生物标志物可能有助于筛选未来初级预防试验的参与者。
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来源期刊
JAMA neurology
JAMA neurology CLINICAL NEUROLOGY-
CiteScore
41.90
自引率
1.70%
发文量
250
期刊介绍: JAMA Neurology is an international peer-reviewed journal for physicians caring for people with neurologic disorders and those interested in the structure and function of the normal and diseased nervous system. The Archives of Neurology & Psychiatry began publication in 1919 and, in 1959, became 2 separate journals: Archives of Neurology and Archives of General Psychiatry. In 2013, their names changed to JAMA Neurology and JAMA Psychiatry, respectively. JAMA Neurology is a member of the JAMA Network, a consortium of peer-reviewed, general medical and specialty publications.
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