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Telomere length, in vivo Alzheimer’s disease pathologies and cognitive decline in older adults

Authors
Jung, Joon HyungByun, Min SooYi, DahyunAhn, HyejinLee, Jun HoLee, Jang-SeokLee, Hyun-SeobLee, Jun-YoungKim, Yu KyeongLee, Yun-SangKang, Koung MiSohn, Chul-HoLee, Dong YoungMook-Jung, InheeChoi, MurimLee, Yu JinHahn, SeokyungKim, Hyun JungChang, Mun YoungLee, Seung HoonHan, Na YoungPae, JisooPark, HansooKim, Jee WookLee, Dong WooLee, Jong-MinSohn, Bo KyungMoon, Seok WooBaek, HyewonKim, Yoon-KeunKim, Jong-WonRyu, Seung-HoKim, Shin GyeomWoo, Jong InnKim, Sang EunCheon, Gi JeongPark, Jee-EunYu, Hyeong GonChoi, Hyo JungChoe, Young MinKim, KwangsooJeon, So YeonKim, Woo JinKo, KangPark, Sung WookJung, GijungJoung, HaejungLee, Han NaByeon, GihwanSung, KiyoungHan, Dong KyunHan, Seung MinKim, Min JungKim, Min JaeKong, NayeongPark, Seo HeeKim, MimiCha, WoojinYeom, HyeryeonChang, Yoon YoungKeum, MusungKim, Min JeongKim, KyungtaeChoi, JeongminChoi, HyejiBae, Han SolSong, Eun SukWoo, DohyunHa, SeunghyukKim, Jun SungKim, Yoon HeePark, SangyongHwang, In AhLee, YejiChoi, YuraGwag, Chung HeeOh, Yoonseok
Issue Date
Jun-2025
Publisher
BMJ Publishing Group
Keywords
ALZHEIMER'S DISEASE; NEUROBIOLOGY; PET; NEUROPATHOLOGY; IMAGE ANALYSIS
Citation
Journal of Neurology, Neurosurgery and Psychiatry, v.96, no.6, pp 558 - 565
Pages
8
Indexed
SCIE
SCOPUS
Journal Title
Journal of Neurology, Neurosurgery and Psychiatry
Volume
96
Number
6
Start Page
558
End Page
565
URI
https://scholarworks.bwise.kr/hanyang/handle/2021.sw.hanyang/210199
DOI
10.1136/jnnp-2024-334314
ISSN
0022-3050
1468-330X
Abstract
Background Whether telomere length (TL), an indicator of biological ageing, reflects Alzheimer’s disease (AD)-related neuropathological change remains unclear. We investigated the relationships between TL, in vivo AD pathologies, including cerebral beta-amyloid and tau deposition, and cognitive outcomes in older adults. Methods A total of 458 older adults were included, encompassing both cognitively normal (CN) individuals and those cognitively impaired (CI), with the CI group consisting of individuals with mild cognitive impairment or AD dementia. All participants underwent clinical and neuropsychological assessments, amyloid positron emission tomography (PET) scan and DNA extraction for measuring TL at baseline. A subset of participants (n=140) underwent tau PET scan. At follow-up, the participants underwent neuropsychological assessments annually for up to 4 years. Results Overall, longer TL was associated with greater brain tau deposition (B=0.139, 95% CI 0.040, 0.238) and a faster decline in global cognition (B = − 0.371, 95% CI − 0.720, –0.023). In the subgroup analysis, the association between longer TL and greater in vivo AD pathologies, as well as faster cognitive decline, was observed particularly in the CI group. Mediation analysis suggested that longer TL was associated with cognitive decline through increased tau deposition in the CI group. Conclusion Our finding suggests that older adults with relatively longer TL, particularly in the CI group, may have greater in vivo AD pathologies and experience more rapid cognitive decline, potentially mediated by brain tau deposition. Further studies are necessary to elucidate the biological links underlying these associations.
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