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Stability in cognitive classification as a function of severity of impairment and ethnicity: A longitudinal analysis.

Authors :
Arruda, Fernanda
Rosselli, Mónica
Mejia Kurasz, Andrea
Loewenstein, David A.
DeKosky, Steven T.
Lang, Merike K.
Conniff, Joshua
Vélez-Uribe, Idaly
Ahne, Emily
Shihadeh, Layaly
Adjouadi, Malek
Goytizolo, Alicia
Barker, Warren W.
Curiel, Rosie E.
Smith, Glenn E.
Duara, Ranjan
Source :
Applied Neuropsychology: Adult. Jun2023, p1-14. 14p. 1 Illustration, 10 Charts.
Publication Year :
2023

Abstract

Abstract Objective Methods Results The interaction of ethnicity, progression of cognitive impairment, and neuroimaging biomarkers of Alzheimer’s Disease remains unclear. We investigated the stability in cognitive status classification (cognitively normal [CN] and mild cognitive impairment [MCI]) of 209 participants (124 Hispanics/Latinos and 85 European Americans).Biomarkers (structural MRI and amyloid PET scans) were compared between Hispanic/Latino and European American individuals who presented a change in cognitive diagnosis during the second or third follow-up and those who remained stable over time.There were no significant differences in biomarkers between ethnic groups in any of the diagnostic categories. The frequency of CN and MCI participants who were progressors (progressed to a more severe cognitive diagnosis at follow-up) and non-progressors (either stable through follow-ups or unstable [progressed but later reverted to a diagnosis of CN]) did not significantly differ across ethnic groups. Progressors had greater atrophy in the hippocampus (HP) and entorhinal cortex (ERC) at baseline compared to unstable non-progressors (reverters) for both ethnic groups, and more significant ERC atrophy was observed among progressors of the Hispanic/Latino group. For European Americans diagnosed with MCI, there were 60% more progressors than reverters (reverted from MCI to CN), while among Hispanics/Latinos with MCI, there were 7% more reverters than progressors. Binomial logistic regressions predicting progression, including brain biomarkers, MMSE, and ethnicity, demonstrated that only MMSE was a predictor for CN participants at baseline. However, for MCI participants at baseline, HP atrophy, ERC atrophy, and MMSE predicted progression. [ABSTRACT FROM AUTHOR]

Details

Language :
English
ISSN :
23279095
Database :
Academic Search Index
Journal :
Applied Neuropsychology: Adult
Publication Type :
Academic Journal
Accession number :
164653558
Full Text :
https://doi.org/10.1080/23279095.2023.2222861