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Clinical Characteristic in Primary Progressive Aphasia in Relation to Alzheimer's Disease Biomarkers

Authors
Kang, Sung HoonCho, HannaShin, JihoKim, Hang-RaiNoh, YoungKim, Eun-JooLyoo, Chul HyoungJang, HyeminKim, Hee JinKoh, Seong-BeomNa, Duk L.Suh, Mee KyungSeo, Sang Won
Issue Date
2021
Publisher
IOS PRESS
Keywords
Amyloid-beta; biomarker; language; primary progressive aphasia; tau
Citation
JOURNAL OF ALZHEIMERS DISEASE, v.84, no.2, pp.633 - 645
Indexed
SCIE
SCOPUS
Journal Title
JOURNAL OF ALZHEIMERS DISEASE
Volume
84
Number
2
Start Page
633
End Page
645
URI
https://scholar.korea.ac.kr/handle/2021.sw.korea/138709
DOI
10.3233/JAD-210392
ISSN
1387-2877
Abstract
Background: Primary progressive aphasia (PPA) is associated with amyloid-beta (A beta) pathology. However, clinical feature of PPA based on A beta positivity remains unclear. Objective: We aimed to assess the prevalence of A beta positivity in patients with PPA and compare the clinical characteristics of patients with A beta-positive (A+) and A beta-negative (A-) PPA. Further, we applied A beta and tau classification system (AT system) in patients with PPA for whom additional information of in vivo tau biomarker was available. Methods: We recruited 110 patients with PPA (41 semantic [svPPA], 27 non-fluent [nfvPPA], 32 logopenic [lvPPA], and 10 unclassified [ucPPA]) who underwent A beta-PET imaging at multi centers. The extent of language impairment and cortical atrophy were compared between the A+ and A- PPA subgroups using general linear models. Results: The prevalence of A beta positivity was highest in patients with lvPPA (81.3%), followed by ucPPA (60.0%), nfvPPA (18.5%), and svPPA (9.8%). The A+PPA subgroup manifested cortical atrophy mainly in the left superior temporal/inferior parietal regions and had lower repetition scores compared to the A-PPA subgroup. Further, we observed that more than 90% (13/14) of the patients with A+PPA had tau deposition. Conclusion: Our findings will help clinicians understand the patterns of language impairment and cortical atrophy in patients with PPA based on A beta deposition. Considering that most of the A+PPA patents are tau positive, understanding the influence of Alzheimer's disease biomarkers on PPA might provide an opportunity for these patients to participate in clinical trials aimed for treating atypical Alzheimer's disease.
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