Identification of differentially expressed genes in post‐mortem tissue from African American Alzheimer disease cases and controls

Identification of differentially expressed genes in post‐mortem tissue from African American Alzheimer disease cases and controls

Background Although the rate of Alzheimer’s disease (AD) in African‐ancestry (AA) Americans is higher than that of persons from European‐ancestry (EA) populations, AA participants have been underrepresented in AD neuropathological studies. Method Utilizing the AD Research Centers (ADRC) infrastructu...

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Veröffentlicht in:Alzheimer's & dementia 2024-12, Vol.20 (S1), p.n/a
Hauptverfasser: Logue, Mark W., Labadorf, Adam Thomas, O'Neill, Nicholas K, Dickson, Dennis W., Flanagan, Margaret E, Franklin, Erin E., Frosch, Matt P., Gearing, Marla, Jin, Lee‐Way, Kofler, Julia, Lee, Eddie B, Mayeux, Richard, McKee, Ann C., Miller, Carol A, Murray, Melissa E., Nelson, Peter T, Perrin, Richard J., Schneider, Julie A., Stein, Thor D., Teich, Andrew F, Troncoso, Juan C, Wang, Shih‐Hsiu Jerry, Mez, Jesse, Farrer, Lindsay A.
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Sprache:eng
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Basic Science and Pathogenesis
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Zusammenfassung:Background Although the rate of Alzheimer’s disease (AD) in African‐ancestry (AA) Americans is higher than that of persons from European‐ancestry (EA) populations, AA participants have been underrepresented in AD neuropathological studies. Method Utilizing the AD Research Centers (ADRC) infrastructure, we obtained AA donor pre‐frontal cortex (PFC) tissue from brain repositories of 12 ADRC and generated bulk RNA sequencing (RNA‐seq) data for 179 samples that met QC and inclusion criteria. Previously generated PFC RNAseq data were obtained for 28 additional AA donors from the Columbia University ADRC. Differential gene expression was evaluated among 125 donors with a neuropathological diagnosis of AD (NIA‐Reagan intermediate or high likelihood) and 82 neuropathologically confirmed controls using regression models including covariates for age at death, sex, cell‐type frequencies, and RNA integrity number (RIN) calculated with Limma. FDR‐corrected p‐values (padj) were calculated to control for the 33,611 genes examined. Result A total of 482 genes surpassed the multiple‐testing threshold. The most significant, ADAMTS2 (p = 2.96 × 10‐8, padj = 0.001), showed increased expression in AD cases (see Table/Figure). We note that ADAMTS2 was differentially expressed in a prior EA study of neuropathologically confirmed AD cases and controls (Panitch et al. Molecular Psychiatry 2021). Additionally, a recent analysis of cognitive resilience in EA neuropathological AD cases identified a strong association with ADAMTS2 (See Li et al. AAIC2024 ). Of the differentially expressed genes observed in the Panitch et al. EA study, 385 (35%) were nominally significant,65 (5.8%) were corrected significant, and most (89%) of these genes had the same effect direction in the AA cohort. Some of the observed associations appear to be AA specific (e.g., EFR3B, IRS4, and CA12; see Table). Additionally, we found nominally significant (p
ISSN:1552-5260
1552-5279
DOI:10.1002/alz.091575