Cerebral Tau Deposition in Comorbid Progressive Supranuclear Palsy and Amyotrophic Lateral Sclerosis: An [18F]-Flortaucipir and 7T MRI Study.

IF 1.9 4区 医学 Q3 CLINICAL NEUROLOGY Neurodegenerative Diseases Pub Date : 2023-01-01 Epub Date: 2024-03-25 DOI:10.1159/000536614
Ian Cheong, Yong Du, Gwenn Smith, Jun Hua, Xu Li, Alexander Pantelyat
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Abstract

Introduction: Progressive supranuclear palsy (PSP) is a four-repeat tauopathy characterized by multiple clinicopathologic subtypes. Advanced neuroimaging techniques have shown an early ability to distinguish PSP subtypes noninvasively for improved diagnosis. This study utilized tau PET imaging and MRI techniques at 7T to determine the neuroimaging profile of a participant with comorbid PSP and amyotrophic lateral sclerosis (ALS).

Method: [18F]-flortaucipir PET imaging was performed on one participant with PSP-ALS, one participant with typical PSP (Richardson's syndrome; PSP-RS), and 15 healthy control volunteers. Standardized uptake value ratio (SUVR) in each brain region was compared between PSP participants and controls. Quantitative susceptibility mapping (QSM) and inflow-based vascular-space occupancy MRI at 7T were performed on the two PSP participants and on two age-matched healthy controls to evaluate for differences in regional brain iron content and arteriolar cerebral blood volume (CBVa), respectively.

Results: In the participant with PSP-ALS, the precentral gyrus demonstrated the highest [18F]-flortaucipir uptake of all brain regions relative to controls (z-score 1.94). In the participant with PSP-RS, [18F]-flortaucipir uptake relative to controls was highest in subcortical regions, including the pallidum, thalamus, hippocampus, and brainstem (z-scores 1.08, 1.41, 1.49, 1.32, respectively). Susceptibility values as a measure of brain iron content were higher in the globus pallidus and substantia nigra than in the midbrain and pons in each participant, regardless of group. CBVa values tended to be higher in the subcortical gray matter in PSP participants than in controls, although large measurement variability was noted in controls across multiple regions.

Conclusion: In vivo tau PET imaging of an individual with PSP-ALS overlap demonstrated increased tau burden in the motor cortex that was not observed in PSP-RS or control participants. Consistent with prior PET studies, tau burden in PSP-RS was mainly observed in subcortical regions, including the brainstem and basal ganglia. QSM data suggest that off-target binding to iron may account for some but not all of the increased [18F]-flortaucipir uptake in the basal ganglia in PSP-RS. These findings support existing evidence that tau PET imaging can distinguish among PSP subtypes by detecting distinct regional patterns of tau deposition in the brain. Larger studies are needed to determine whether CBVa is sensitive to changes in brain microvasculature in PSP.

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共病进行性核上性麻痹和肌萎缩侧索硬化症的脑tau沉积:[18F]-flortaucipir和7T磁共振成像研究。
导言:进行性核上性麻痹(PSP)是一种四重复tauopathy,具有多种临床病理亚型。先进的神经影像学技术已显示出早期无创区分 PSP 亚型以改善诊断的能力。本研究利用 tau-PET 成像和 7 特斯拉(7T)核磁共振成像技术确定了一名合并 PSP 和肌萎缩侧索硬化症(ALS)患者的神经影像学特征。该方法对一名 PSP-ALS 患者、一名典型 PSP(理查森综合征;PSP-RS)患者和 15 名健康对照志愿者进行了[18F]-flortaucipir PET 成像检查。比较了 PSP 患者和对照组每个脑区的标准化摄取值比(SUVR)。在 7T 下对两名 PSP 患者和两名年龄匹配的健康对照者进行了定量易感性映射(QSM)和基于流入的血管空间占位(iVASO)磁共振成像,以分别评估区域脑铁含量和动脉脑血容量(CBVa)的差异。结果 在 PSP-ALS 患者中,相对于对照组,前中央回的[18F]-flortaucipir 摄取量在所有脑区中最高(z-score 1.94)。在 PSP-RS 患者中,皮层下区域(包括苍白球、丘脑、海马和脑干)的[18F]-flortaucipir 摄取量相对于对照组最高(z 值分别为 1.08、1.41、1.49 和 1.32)。作为脑铁含量的测量指标,每位受试者的球状苍白球和黑质的易感性值均高于中脑和脑桥,与组别无关。与对照组相比,PSP 参与者皮层下灰质中的 CBVa 值往往更高,但对照组在多个区域的测量结果差异较大。结论 对一名PSP-ALS重叠患者进行的体内tau PET成像显示,运动皮层中的tau负荷增加,而在PSP-RS或对照组患者中未观察到这一现象。与之前的 PET 研究一致,PSP-RS 患者的 tau 负荷主要出现在皮层下区域,包括脑干和基底节。QSM数据表明,与铁的脱靶结合可能是PSP-RS基底节中[18F]-flortaucipir摄取增加的部分原因,但不是全部原因。这些发现支持现有的证据,即 tau PET 成像可以通过检测大脑中不同区域的 tau 沉积模式来区分 PSP 亚型。还需要进行更大规模的研究,以确定CBVa对PSP患者脑微血管的变化是否敏感。
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来源期刊
Neurodegenerative Diseases
Neurodegenerative Diseases 医学-临床神经学
CiteScore
5.90
自引率
0.00%
发文量
14
审稿时长
6-12 weeks
期刊介绍: ''Neurodegenerative Diseases'' is a bimonthly, multidisciplinary journal for the publication of advances in the understanding of neurodegenerative diseases, including Alzheimer''s disease, Parkinson''s disease, amyotrophic lateral sclerosis, Huntington''s disease and related neurological and psychiatric disorders.
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