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APOE ϵ4 Increases Risk for Dementia in Pure Synucleinopathies

Debby W. TsuangVeterans Affairs Puget Sound Health Care System, Seattle,WA98108, USAJames B. LeverenzUniversity of WashingtonOscar L. LópezUniversity of PittsburghRonald L. HamiltonUniversity of PittsburghDavid A. BennettRush UniversityJulie A. SchneiderRush UniversityAron S. BuchmanRush UniversityEric B. LarsonUniversity of WashingtonPaul K. CraneUniversity of WashingtonJeffrey KayeOregon Health and Science UniversityPatricia KramerOregon Health and Science UniversityRandy WoltjerOregon Health and Science UniversityJohn Q. Trojanowski#N# * University of PennsylvaniaDaniel WeintraubVA Medical CenterAlice Chen‐Plotkin#N# * University of PennsylvaniaDavid J. Irwin#N# * University of PennsylvaniaJacqueline RickUniversity of PennsylvaniaGerard D. Schellenberg#N# * University of PennsylvaniaG. Stennis WatsonUniversity of WashingtonWalter A. KukullUniversity of WashingtonPeter T. Nelson#N##TAB##TAB##TAB##TAB# Univ. of Kentucky#N##TAB##TAB##TAB#Gregory A. Jicha#N##TAB##TAB##TAB##TAB# Univ. of Kentucky#N##TAB##TAB##TAB#Janna H. Neltner#N##TAB##TAB##TAB##TAB# Univ. of Kentucky#N##TAB##TAB##TAB#Doug GalaskoUniversity of California at San DiegoEliezer MasliahUniversity of California at San DiegoJoseph F. QuinnKathryn A. ChungDora YearoutUniversity of WashingtonIgnácio F. MataUniversity of WashingtonJia Y. WanUniversity of WashingtonKaren L. EdwardsUniversity of WashingtonThomas J. MontineUniversity of WashingtonCyrus P. ZabetianUniversity of Washington
2012en
ABI

Annotatsiya

OBJECTIVE: To test for an association between the apolipoprotein E (APOE) ϵ4 allele and dementias with synucleinopathy. DESIGN: Genetic case-control association study. SETTING: Academic research. PATIENTS: Autopsied subjects were classified into 5 categories: dementia with high-level Alzheimer disease (AD) neuropathologic changes (NCs) but without Lewy body disease (LBD) NCs (AD group; n=244), dementia with LBDNCs and high-level ADNCs (LBD-AD group; n=224), dementia with LBDNCs and no or low levels of ADNCs (pure DLB [pDLB] group; n=91), Parkinson disease dementia (PDD) with no or low levels of ADNCs (n=81), and control group (n=269). MAIN OUTCOME MEASURE The APOE allele frequencies. RESULTS The APOE ϵ4 allele frequency was significantly higher in the AD (38.1%), LBD-AD (40.6%), pDLB (31.9%), and PDD (19.1%) groups compared with the control group (7.2%; overall χ(2)(4)=185.25; P=5.56 × 10(-39)), and it was higher in the pDLB group than the PDD group (P= .01). In an age-adjusted and sex-adjusted dominant model, ϵ4 was strongly associated with AD (odds ratio, 9.9; 95% CI, 6.4-15.3), LBD-AD (odds ratio, 12.6; 95% CI, 8.1-19.8), pDLB (odds ratio, 6.1; 95% CI, 3.5-10.5), and PDD (odds ratio, 3.1; 95% CI, 1.7-5.6). CONCLUSIONS The APOE ϵ4 allele is a strong risk factor across the LBD spectrum and occurs at an increased frequency in pDLB relative to PDD. This suggests that ϵ4 increases the likelihood of presenting with dementia in the context of a pure synucleinopathy. The elevated ϵ4 frequency in the pDLB and PDD groups, in which the overall brain neuritic plaque burden was low, indicates that apoE might contribute to neurodegeneration through mechanisms unrelated to amyloid processing.

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