Investigation of the independent role of a rare APOE variant (L28P; APOE*4Pittsburgh) in late-onset Alzheimer disease.

TitleInvestigation of the independent role of a rare APOE variant (L28P; APOE*4Pittsburgh) in late-onset Alzheimer disease.
Publication TypeJournal Article
Year of Publication2023
AuthorsFan KH, Francis L, M Aslam M, Bedison MA, Lawrence E, Acharya V, Snitz BE, Ganguli M, DeKosky ST, Lopez OL, Feingold E, M Kamboh I
JournalNeurobiol Aging
Volume122
Pagination107-111
Date Published02/2023
ISSN1558-1497
KeywordsAlleles, Alzheimer Disease, Animals, Apolipoprotein E3, Apolipoprotein E4, Apolipoproteins E, Genotype, Heterozygote
Abstract

A rare missense APOE variant (L28P; APOE*4Pittsburgh), which is present only in populations with European ancestry, has been reported to be a risk factor for late-onset Alzheimer's disease (LOAD). However, due to the complete linkage disequilibrium of L28P with APOE*4 (C112R), its independent genetic association is uncertain. The original association study implicating L28P with LOAD risk was carried out in a relatively small sample size. In the current study, we have re-evaluated this association in a large case-control sample of 15,762 White U.S. subjects and investigated its independent effect in APOE 3/4 subjects, as L28P has been observed only in the heterozygous state of APOE*4 carriers and 3/4 is the most common genotype containing the APOE*4 allele. The heterozygous carrier frequency of L28P, all with APOE*4, was about 3-fold higher in AD cases than in cognitively intact controls (0.845% vs. 0.277%). The age- and sex-adjusted meta-analysis odds ratio (OR) was 2.87 (95% CI: 1.34 - 6.13; = 0.0066). Among APOE 3/4 subjects, age- and sex-adjusted meta-analysis OR was 1.53 (95% CI: 0.70 - 3.36; p = 0.28), indicating its effect was independent of APOE*4. The lack of statistical significance appears mainly due to the low power of 4138 subjects with the 3/4 genotype (12% power at α= 0.05) compared to the required sample of 139,088 subjects with the 3/4 genotype to detect an OR of 1.5 at α= 0.05 and 80% power. Our data suggesting that L28P has an independent genetic effect on AD risk is reinforced by earlier experimental findings showing that this mutation leads to significant structural and conformational changes in the ApoE4 molecule and can induce functional defects associated with neuronal Aβ42 accumulation and oxidative stress. Additional functional studies in cell-based systems and animal models will help to delineate its functional significance in the etiology of AD.
DOI10.1016/j.neurobiolaging.2022.11.007
Alternate JournalNeurobiol Aging
PubMed ID36528961
PubMed Central IDPMC9839598
Grant ListU01 AG049506 / AG / NIA NIH HHS / United States
R01 AG023629 / AG / NIA NIH HHS / United States
U01 AG057659 / AG / NIA NIH HHS / United States
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HHSN268201100012C / HL / NHLBI NIH HHS / United States
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HHSN268201100010C / HL / NHLBI NIH HHS / United States
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HHSN268201100008C / HL / NHLBI NIH HHS / United States
N01HC85080 / HL / NHLBI NIH HHS / United States
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U01 HL080295 / HL / NHLBI NIH HHS / United States
U01 AT000162 / AT / NCCIH NIH HHS / United States
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HHSN268201100007C / HL / NHLBI NIH HHS / United States
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R37 AG023651 / AG / NIA NIH HHS / United States
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U01 AG016976 / AG / NIA NIH HHS / United States
N01HC85082 / HL / NHLBI NIH HHS / United States
T32 MH019986 / MH / NIMH NIH HHS / United States
HHSN268201500001I / HL / NHLBI NIH HHS / United States
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N01HC55222 / HL / NHLBI NIH HHS / United States
R01 AG054076 / AG / NIA NIH HHS / United States
U24 AG041689 / AG / NIA NIH HHS / United States
N01HC85079 / HL / NHLBI NIH HHS / United States
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P50 AG005133 / AG / NIA NIH HHS / United States
UF1 AG047133 / AG / NIA NIH HHS / United States
N01HC25195 / HL / NHLBI NIH HHS / United States
U54 HG003067 / HG / NHGRI NIH HHS / United States
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HHSN268201100005C / HL / NHLBI NIH HHS / United States
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R01 AG015928 / AG / NIA NIH HHS / United States
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HHSN268201100009C / HL / NHLBI NIH HHS / United States
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