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Distinct <SUP>11</SUP>C-ER176 PET Neuroinflammatory Profiles and Tau Colocalization in Progressive Apraxia of Speech With and Without Parkinson-plus SyndromeDistinct 11C-ER176 PET Neuroinflammatory Profiles and Tau Colocalization in Progressive Apraxia of Speech With and Without Parkinson-plus Syndrome

Other Titles
Distinct 11C-ER176 PET Neuroinflammatory Profiles and Tau Colocalization in Progressive Apraxia of Speech With and Without Parkinson-plus Syndrome
Authors
Satoh, RyotaUtianski, Rene L.Duffy, Joseph R.Clark, Heather M.Stephens, Yehkyoung C.Lee, JeyeonBaker, MattRademakers, RosaLowe, Val J.Josephs, Keith A.Whitwell, Jennifer L.
Issue Date
Aug-2025
Publisher
Lippincott Williams & Wilkins Ltd.
Keywords
apraxia of speech; neuroinflammation; C-11-ER176; CBS; PSP
Citation
Clinical Nuclear Medicine, v.50, no.8, pp 731 - 742
Pages
12
Indexed
SCIE
SCOPUS
Journal Title
Clinical Nuclear Medicine
Volume
50
Number
8
Start Page
731
End Page
742
URI
https://scholarworks.bwise.kr/hanyang/handle/2021.sw.hanyang/208337
DOI
10.1097/RLU.0000000000005962
ISSN
0363-9762
1536-0229
Abstract
Background: Progressive apraxia of speech (PAOS) is a neurodegenerative disorder most commonly arising from a 4-repeat tauopathy that affects the programming or planning of speech, although many patients develop a Parkinson-plus syndrome. The role of neuroinflammation as a disease mechanism is unknown. We investigated the spatial pattern of neuroinflammation in PAOS using PET and evaluated whether it is associated with disease severity, presence of Parkinson-plus features, and tau PET uptake. Patients and Methods: Twenty-five PAOS patients (13 with Parkinson-plus features) and 30 controls underwent inflammatory C-11-ER176 and tau F-18-flortaucipir PET scans as well as detailed clinical assessments. Multiple linear regression analyses compared the inflammatory standardized uptake value ratio (SUVR) between PAOS and controls and assessed the relationship with clinical test scores. Pearson correlation analysis examined the relationship between inflammatory and tau SUVRs. Results: PAOS had greater neuroinflammatory SUVR than controls in the precentral, supplementary motor area, frontal gyri, putamen, pallidum, subthalamic nucleus, and red nucleus (adjusted P < 0.05). Greater neuroinflammation was associated with worse parkinsonism, and patients who had developed Parkinson-plus features showed a broader pattern of neuroinflammation, extending to prefrontal, temporal and parietal cortices. Neuroinflammation correlated with tau uptake in most (96%) PAOS patients (r > 0.3, P < 0.05). The higher correlation was associated with worse parkinsonism (r = 0.61, P < 0.05) and disease severity (r = 0.54, P < 0.05). Conclusions: C-11-ER176 PET analysis demonstrates neuroinflammation in frontal and subcortical regions in PAOS which is particularly severe and widespread with the development of Parkinson-plus clinical features. The colocalization of neuroinflammation and tau may support a relationship between these disease mechanisms.
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서울 의과대학 (DEPARTMENT OF BIOMEDICAL ENGINEERING)
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