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早期 tau 在 flortaucipir 影像中的检测:在尸检确认数据中的验证及其对疾病进展的影响。

Early tau detection in flortaucipir images: validation in autopsy-confirmed data and implications for disease progression.

机构信息

Eli Lilly and Company, Indianapolis, IN, 46285, USA.

出版信息

Alzheimers Res Ther. 2023 Feb 28;15(1):41. doi: 10.1186/s13195-023-01160-6.

Abstract

BACKGROUND

There is an increasing interest in utilizing tau PET to identify patients early in Alzheimer's disease (AD). In this work, a temporal lobe composite (Eτ) volume of interest (VOI) was evaluated in a longitudinal flortaucipir cohort and compared to a previously described global neocortical VOI. In a separate autopsy-confirmed study, the sensitivity of the Eτ VOI for identifying intermediate (B2) neurofibrillary tangle (NFT) pathology was evaluated.

METHODS

A total of 427 subjects received flortaucipir, florbetapir, MRI, and cognitive evaluation at baseline and 18 months. In a separate autopsy study, 67 subjects received ante-mortem flortaucipir scans, and neuropathological findings were recorded according to NIA-AA recommendations by two experts. Two VOIs: Eτ comprising FreeSurfer volumes (bilateral entorhinal cortex, fusiform, parahippocampal, and inferior temporal gyri) transformed to MNI space and a previously published global AD signature-weighted neocortical VOI (AD) (Devous et al., J Nucl Med 59:937-43, 2018), were used to calculate SUVr relative to a white matter reference region (PERSI) (Southekal et al., J Nucl Med Off Publ Soc Nucl Med 59:944-51, 2018). SUVr cutoffs for positivity were determined based on a cohort of young, cognitively normal subjects. Subjects were grouped based on positivity on both VOIs (Eτ+/AD+; Eτ+/AD-; Eτ-/AD-). Groupwise comparisons were performed for baseline SUVr, 18-month changes in SUVr, neurodegeneration, and cognition. For the autopsy study, the sensitivity of Eτ in identifying intermediate Braak pathology (B2) subjects was compared to that of AD signature-weighted neocortical VOI. The average surface maps of subjects in the Eτ+/AD- group and B2 NFT scores were created for visual evaluation of uptake.

RESULTS

Sixty-four out of 390 analyzable subjects were identified as Eτ+/AD-: 84% were Aβ+, 100% were diagnosed as MCI or AD, and 59% were APOE ε4 carriers. Consistent with the hypothesis that Eτ+/AD- status reflects an early stage of AD, Eτ+/AD- subjects deteriorated significantly faster than Eτ-/AD- subjects, but significantly slower than Eτ+/AD+ subjects, on most measures (i.e., change in AD SUVr, Eτ ROI cortical thickness, and MMSE). The AD VOI was selective for subjects who came to autopsy with a B3 NFT score. In the autopsy study, 12/15 B2 subjects (including 10/11 Braak IV) were Eτ+/AD-. Surface maps showed that flortaucipir uptake was largely captured by the Eτ VOI regions in B2 subjects.

CONCLUSION

The Eτ VOI identified subjects with elevated temporal but not global tau (Eτ+/AD-) that were primarily Aβ+, APOE ε4 carriers, and diagnosed as MCI or AD. Eτ+/AD- subjects had greater accumulation of tau, greater atrophy, and higher decline on MMSE in 18 months compared to Eτ-/AD- subjects. Finally, the Eτ VOI identified the majority of the intermediate NFT score subjects in an autopsy-confirmed study. As far as we know, this is the first study that presents a visualization of ante-mortem FTP retention patterns that at a group level agree with the neurofibrillary tangle staging scheme proposed by Braak. These findings suggest that the Eτ VOI may be sensitive for detecting impaired subjects early in the course of Alzheimer's disease.

摘要

背景

利用 tau PET 来识别阿尔茨海默病(AD)早期患者的兴趣日益增加。在这项工作中,在纵向 flortaucipir 队列中评估了颞叶复合(Eτ)体积感兴趣区(VOI),并与之前描述的全局新皮质 VOI 进行了比较。在一项单独的尸检证实研究中,评估了 Eτ VOI 识别中间(B2)神经纤维缠结(NFT)病理学的敏感性。

方法

共有 427 名受试者在基线和 18 个月时接受了 flortaucipir、florbetapir、MRI 和认知评估。在一项单独的尸检研究中,67 名受试者接受了生前 flortaucipir 扫描,根据 NIA-AA 建议,两名专家记录了神经病理学发现。使用两个 VOI:包含 FreeSurfer 体积(双侧内嗅皮层、梭状回、海马旁回和颞下回)转换为 MNI 空间的 Eτ 和以前发表的全局 AD 特征加权新皮质 VOI(AD)(Devous 等人,J Nucl Med 59:937-43, 2018),用于计算相对于白质参考区域(PERSI)的 SUVr(Southekal 等人,J Nucl Med Off Publ Soc Nucl Med 59:944-51, 2018)。根据年轻、认知正常受试者的队列确定了阳性的 SUVr 截止值。根据两个 VOI(Eτ+/AD+;Eτ+/AD-;Eτ-/AD-)的阳性情况对受试者进行分组。进行了基线 SUVr、18 个月 SUVr 变化、神经退行性变和认知的组间比较。对于尸检研究,比较了 Eτ 识别中间 Braak 病理学(B2)受试者的敏感性与 AD 特征加权新皮质 VOI。为了视觉评估摄取,为 Eτ+/AD-组的受试者创建了平均表面图和 B2 NFT 评分。

结果

在 390 名可分析的受试者中,有 64 名被确定为 Eτ+/AD-:84%为 Aβ+,100%被诊断为 MCI 或 AD,59%为 APOE ε4 携带者。与 Eτ+/AD-状态反映 AD 早期阶段的假设一致,Eτ+/AD-受试者在大多数指标(即 AD SUVr、Eτ ROI 皮质厚度和 MMSE 的变化)上的恶化速度明显快于 Eτ-/AD-受试者,但明显慢于 Eτ+/AD+受试者。AD VOI 对尸检时出现 B3 NFT 评分的受试者具有选择性。在尸检研究中,12/15 名 B2 受试者(包括 10/11 名 Braak IV)为 Eτ+/AD-。表面图显示,flortaucipir 的摄取主要被 B2 受试者的 Eτ VOI 区域捕获。

结论

Eτ VOI 识别出具有升高的颞叶但没有全局 tau(Eτ+/AD-)的受试者,这些受试者主要为 Aβ+、APOE ε4 携带者,并被诊断为 MCI 或 AD。与 Eτ-/AD-受试者相比,Eτ+/AD-受试者在 18 个月内具有更大的 tau 积累、更大的萎缩和更高的 MMSE 下降。最后,Eτ VOI 在尸检证实的研究中识别出了大多数中间 NFT 评分受试者。据我们所知,这是第一项展示生前 FTP 保留模式的研究,这些模式在群体水平上与 Braak 提出的神经纤维缠结分期方案一致。这些发现表明,Eτ VOI 可能对检测阿尔茨海默病早期的受损患者敏感。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/12da/9972744/cd326f3f2a21/13195_2023_1160_Fig1_HTML.jpg

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