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血浆P-tau217在记忆门诊早期阿尔茨海默病患者中评估淀粉样蛋白降低免疫治疗适用性的临床应用

Clinical application of plasma P-tau217 to assess eligibility for amyloid-lowering immunotherapy in memory clinic patients with early Alzheimer's disease.

作者信息

Howe Matthew D, Britton Karysa J, Joyce Hannah E, Menard William, Emrani Sheina, Kunicki Zachary J, Faust Melanie A, Dawson Brittany C, Riddle Meghan C, Huey Edward D, Janelidze Shorena, Hansson Oskar, Salloway Stephen P

出版信息

Res Sq. 2024 May 29:rs.3.rs-3755419. doi: 10.21203/rs.3.rs-3755419/v1.

Abstract

BACKGROUND

With the approval of disease-modifying treatments (DMTs) for early Alzheimer's disease (AD), there is an increased need for efficient and non-invasive detection methods for cerebral amyloid-β (Aβ) pathology. Current methods, including positron emission tomography (PET) and cerebrospinal fluid (CSF) analysis, are costly and invasive methods that may limit access to new treatments. Plasma tau phosphorylated at threonine-217 (P-tau217) presents a promising alternative, yet optimal cutoffs for treatment eligibility with DMTs like aducanumab require further investigation. This study evaluates the efficacy of one- and two-cutoff strategies for determining DMT eligibility at the Butler Hospital Memory & Aging Program (MAP).

METHODS

In this retrospective, cross-sectional diagnostic cohort study, we first developed P-tau217 cutoffs using site-specific training data and BioFINDER-2, which were then tested in potential DMT candidates from Butler MAP (total n = 150). ROC analysis was used to calculate the area under the curve (AUC) and accuracy of P-tau217 interpretation strategies, using Aβ-PET/CSF testing as the standard of truth.

RESULTS

Potential DMT candidates at Butler MAP (n = 50), primarily diagnosed with mild cognitive impairment (n = 29 [58%]) or mild dementia (21 [42%]), were predominantly Aβ-positive (38 [76%]), and half (25 [50%]) were subsequently treated with aducanumab. Elevated P-tau217 predicted cerebral Aβ positivity in potential DMT candidates (AUC = 0.97 [0.92-1]), with diagnostic accuracy ranging from 0.88 (0.76-0.95, p = 0.028) to 0.96 (0.86-1, p < .001). When using site-specific cutoffs, a subset of DMT candidates (10%) exhibited borderline P-tau217 (between 0.273 and 0.399 pg/mL) that would have potentially required from confirmatory testing.

CONCLUSIONS

This study, which included participants treated with aducanumab, confirms the utility of one- and two-cutoff strategies for interpreting plasma P-tau217 in assessing DMT eligibility. Using P-tau217 could potentially replace more invasive diagnostic methods, and all aducanumab-treated participants would have been deemed eligible based on P-tau217. However, false positives remain a concern, particularly when applying externally derived cutoffs that exhibited lower specificity which could have led to inappropriate treatment of Aβ-negative participants. Future research should focus on prospective validation of P-tau217 cutoffs to enhance their generalizability and inform standardized treatment decision-making across diverse populations.

摘要

背景

随着针对早期阿尔茨海默病(AD)的疾病修饰治疗(DMTs)获得批准,对脑淀粉样β(Aβ)病理的高效、非侵入性检测方法的需求日益增加。目前的方法,包括正电子发射断层扫描(PET)和脑脊液(CSF)分析,成本高且具有侵入性,可能会限制获得新治疗的机会。苏氨酸-217位点磷酸化的血浆tau蛋白(P-tau217)是一种有前景的替代方法,但对于像阿杜卡单抗这样的DMTs,确定治疗资格的最佳临界值需要进一步研究。本研究评估了巴特勒医院记忆与衰老项目(MAP)中用于确定DMT资格的单临界值和双临界值策略的有效性。

方法

在这项回顾性横断面诊断队列研究中,我们首先使用特定地点的训练数据和BioFINDER-2开发了P-tau217临界值,然后在巴特勒MAP的潜在DMT候选者中进行测试(总共n = 150)。以Aβ-PET/CSF检测作为金标准,采用ROC分析来计算曲线下面积(AUC)和P-tau217解读策略的准确性。

结果

巴特勒MAP的潜在DMT候选者(n = 50),主要诊断为轻度认知障碍(n = 29 [58%])或轻度痴呆(21 [42%]),大多为Aβ阳性(38 [76%]),其中一半(25 [50%])随后接受了阿杜卡单抗治疗。P-tau217升高预测了潜在DMT候选者的脑Aβ阳性(AUC = 0.97 [0.92 - 1]),诊断准确性范围为0.88(0.76 - 0.95,p = 0.028)至0.96(0.86 - 1,p <.001)。当使用特定地点的临界值时,一部分DMT候选者(10%)的P-tau217处于临界值(0.273至0.399 pg/mL之间),这可能需要进行确认性检测。

结论

本研究纳入了接受阿杜卡单抗治疗的参与者,证实了单临界值和双临界值策略在评估DMT资格时解读血浆P-tau217的效用。使用P-tau217可能会取代侵入性更强的诊断方法,并且所有接受阿杜卡单抗治疗的参与者基于P-tau217都可能被视为符合资格。然而,假阳性仍然是一个问题,特别是在应用外部得出的临界值时,这些临界值显示出较低的特异性,可能导致对Aβ阴性参与者进行不适当的治疗。未来的研究应专注于P-tau217临界值的前瞻性验证,以提高其通用性,并为不同人群的标准化治疗决策提供依据。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/96f3/11160917/7a9215ea1844/nihpp-rs3755419v1-f0001.jpg

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