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Cited 6 time in webofscience Cited 6 time in scopus
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Apolipoprotein epsilon 7 allele in memory complaints: insights through protein structure prediction

Authors
Youn, Young ChulLim, Yong KwanHan, Su-HyunGiau, Vo VanLee, Mi-KyungPark, Kwang-YeolKim, Sang YunBagyinszky, EvaAn, Seong Soo AKim, Hye Ryoun
Issue Date
Jul-2017
Publisher
DOVE MEDICAL PRESS LTD
Keywords
apolipoprotein structure; Alzheimer's disease; vascular cognitive impairment; small vessel disease
Citation
CLINICAL INTERVENTIONS IN AGING, v.12, pp 1095 - 1102
Pages
8
Journal Title
CLINICAL INTERVENTIONS IN AGING
Volume
12
Start Page
1095
End Page
1102
URI
https://scholarworks.bwise.kr/cau/handle/2019.sw.cau/6255
DOI
10.2147/CIA.S131172
ISSN
1178-1998
1178-1998
Abstract
Purpose: APOE epsilon 7 gene is a rare mutant form of APOE epsilon 3. The mutation occurs in the lipid-binding domain of APOE. Based on the protein's structure, APOE epsilon 7 is expected to function in lipid and beta-amyloid metabolism, similar to APOE epsilon 4. However, unlike that for APOE kappa 4, the mechanisms responsible for Alzheimer's disease (AD) cases associated with APOE epsilon 7 expression have not been elucidated. The present study aims to investigate the association between APOE epsilon 7 expression and cognitive impairment. Methods: APOE was sequenced in DNA samples collected from 344 memory-complaint patients who visited the memory clinic, and from 345 non-memory-complaint individuals from the health promotion center. The protein structures of ApoE3, ApoE4, and ApoE7 were predicted. Results: Three epsilon 3/epsilon 7 heterozygote individuals who were all classified under the memorycomplaint group were identified. Of these, two subjects were clinically diagnosed with AD with small vessel disease, and the remaining individual was diagnosed with subjective cognitive impairment. This study predicted the protein structures of ApoE3, ApoE4, and ApoE7 and determined the three-dimensional structure of the carboxy terminus of ApoE7, which participates in an electrostatic domain interaction similar to that of APOE epsilon 4. APOE K244 or K245 mutations for APOE e7 were not found in the Korean reference genome database, which contains information (http://152.99.75.168/KRGDB/browser/mainBrowser. jsp) from 622 healthy individuals. Conclusion: As verified by the results of structural prediction, APOE epsilon 7 could serve as another risk factor for cognitive impairment and is particularly associated with vascular disease. However, additional studies are required to validate the pathogenic nature of APOE epsilon 7.
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