Why Inclusion Matters for Alzheimer's Disease Biomarker Discovery in Plasma

Overview

Journal J Alzheimers Dis

Publisher Sage Publications

Specialties Geriatrics
Neurology

Date 2021 Jan 11

PMID 33427747

Citations 20

Authors

Mostafa J Khan

Heather Desaire

Oscar L Lopez

M Ilyas Kamboh

Rena A S Robinson

Affiliations

Soon will be listed here.

Abstract

Background: African American/Black adults have a disproportionate incidence of Alzheimer's disease (AD) and are underrepresented in biomarker discovery efforts.

Objective: This study aimed to identify potential diagnostic biomarkers for AD using a combination of proteomics and machine learning approaches in a cohort that included African American/Black adults.

Methods: We conducted a discovery-based plasma proteomics study on plasma samples (N = 113) obtained from clinically diagnosed AD and cognitively normal adults that were self-reported African American/Black or non-Hispanic White. Sets of differentially-expressed proteins were then classified using a support vector machine (SVM) to identify biomarker candidates.

Results: In total, 740 proteins were identified of which, 25 differentially-expressed proteins in AD came from comparisons within a single racial and ethnic background group. Six proteins were differentially-expressed in AD regardless of racial and ethnic background. Supervised classification by SVM yielded an area under the curve (AUC) of 0.91 and accuracy of 86%for differentiating AD in samples from non-Hispanic White adults when trained with differentially-expressed proteins unique to that group. However, the same model yielded an AUC of 0.49 and accuracy of 47%for differentiating AD in samples from African American/Black adults. Other covariates such as age, APOE4 status, sex, and years of education were found to improve the model mostly in the samples from non-Hispanic White adults for classifying AD.

Conclusion: These results demonstrate the importance of study designs in AD biomarker discovery, which must include diverse racial and ethnic groups such as African American/Black adults to develop effective biomarkers.

Citing Articles

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Alzheimer's disease CSF biomarkers correlate with early pathology and alterations in neuronal and glial gene expression.

Ropri A, Lam T, Kalia V, Buchanan H, Bartosch A, Youth E Alzheimers Dement. 2024; 20(10):7090-7103.

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Clinical application of plasma P-tau217 to assess eligibility for amyloid-lowering immunotherapy in memory clinic patients with early Alzheimer's disease.

Howe M, Britton K, Joyce H, Menard W, Emrani S, Kunicki Z Alzheimers Res Ther. 2024; 16(1):154.

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Alzheimer's disease CSF biomarkers correlate with early pathology and alterations in neuronal and glial gene expression.

Ropri A, Lam T, Kalia V, Buchanan H, Bartosch A, Youth E medRxiv. 2024; .

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Clinical application of plasma P-tau217 to assess eligibility for amyloid-lowering immunotherapy in memory clinic patients with early Alzheimer's disease.

Howe M, Britton K, Joyce H, Menard W, Emrani S, Kunicki Z Res Sq. 2024; .

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