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Association between APOE ε2 and Aβ burden in patients with Alzheimer- and vascular-type cognitive impairmentopen accessAssociation between <i>APOE</i> ε2 and Aβ burden in patients with Alzheimer- and vascular-type cognitive impairment

Other Titles
Association between <i>APOE</i> ε2 and Aβ burden in patients with Alzheimer- and vascular-type cognitive impairment
Authors
Lee, Jin SanLee, HyejooPark, SeongbeomChoe, YeongsimPark, Yu HyunCheon, Bo KyoungHahn, AliceOssenkoppele, RikKim, Hee JinKim, SeonwooYoo, HeejinJang, HyeminCho, Soo HyunKim, Seung JooKim, Jun PyoJung, Young HeePark, Key-ChungDeCarli, CharlesWeiner, Michael W.Na, Duk L.Seo, Sang Won
Issue Date
Oct-2020
Publisher
Lippincott Williams & Wilkins Ltd.
Citation
Neurology, v.95, no.17, pp E2354 - E2365
Indexed
SCIE
SCOPUS
Journal Title
Neurology
Volume
95
Number
17
Start Page
E2354
End Page
E2365
URI
https://scholarworks.gnu.ac.kr/handle/sw.gnu/72336
DOI
10.1212/WNL.0000000000010811
ISSN
0028-3878
1526-632X
Abstract
Objective To investigate the association between APOE genotype and beta-amyloid (A beta) burden, as measured by PET in patients with subcortical vascular cognitive impairment (SVCI) and those with Alzheimer disease-related cognitive impairment (ADCI). Methods This was a cross-sectional study of 310 patients with SVCI and 999 with ADCI. To evaluate the effects of APOE genotype or diagnostic group on A beta positivity, we performed multivariate logistic regression analyses. Further distinctive underlying features of latent subgroups were examined by employing a latent class cluster analysis approach. Results In comparison with epsilon 3 homozygotes, in the ADCI group, epsilon 2 carriers showed a lower frequency of A beta positivity (odds ratio [OR] 0.43, 95% confidence interval [CI] 0.23-0.79), while in the SVCI group, epsilon 2 carriers showed a higher frequency of A beta positivity (OR 2.26, 95% CI 1.02-5.01). In particular, we observed an interaction effect of epsilon 2 carrier status and diagnostic group on A beta positivity (OR 5.12, 95% CI 1.93-13.56), in that relative to epsilon 3 homozygotes, there were more A beta-positive epsilon 2 carriers in the SVCI group than in the ADCI group. We also identified latent subgroups of A beta-positive APOE epsilon 2 carriers with SVCI and A beta-positive APOE epsilon 4 carriers with ADCI. Conclusions Our findings suggest that APOE epsilon 2 is distinctly associated with A beta deposition in patients with SVCI and those with ADCI. Our findings further suggest that there is a distinctive subgroup of A beta-positive APOE epsilon 2 carriers with SVCI among patients with cognitive impairment.
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