Neuropsychological and clinical variables associated with cognitive trajectories in patients with Alzheimer's disease

BackgroundThe NeuroArtP3 (NET-2018-12366666) is a multicenter study funded by the Italian Ministry of Health. The aim of the project is to identify the prognostic trajectories of Alzheimer's disease (AD) through the application of artificial intelligence (AI). Only a few AI studies investigated...

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Main Authors: Marianna Riello, Monica Moroni, Stefano Bovo, Flavio Ragni, Manuela Buganza, Raffaella Di Giacopo, Marco Chierici, Lorenzo Gios, Matteo Pardini, Federico Massa, Monica Dallabona, Elisa Vanzetta, Cristina Campi, Michele Piana, Sara Garbarino, Manuela Marenco, Venet Osmani, Giuseppe Jurman, Antonio Uccelli, Bruno Giometto, NeuroArtP3 Network, Filippo Gerli, Guido Pasquini, Claudia Niccolai, Matteo Betti, Emilio Portaccio, Maria Pia Amato, Rossi Andrea, Parodi Costanza, Ramaglia Antonia, Tortora Domenico, Severino Mariasavina, Andrea Falini, Antonella Castellano, Nicolò Pecco, Paola Scifo, Sonia Calloni
Format: Article
Language:English
Published: Frontiers Media S.A. 2025-05-01
Series:Frontiers in Aging Neuroscience
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Online Access:https://www.frontiersin.org/articles/10.3389/fnagi.2025.1565006/full
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Summary:BackgroundThe NeuroArtP3 (NET-2018-12366666) is a multicenter study funded by the Italian Ministry of Health. The aim of the project is to identify the prognostic trajectories of Alzheimer's disease (AD) through the application of artificial intelligence (AI). Only a few AI studies investigated the clinical variables associated with cognitive worsening in AD. We used Mini Mental State Examination (MMSE) scores as outcome to identify the factors associated with cognitive decline at follow up.MethodsA sample of N = 126 patients diagnosed with AD (MMSE >19) were followed during 3 years in 4 time-points: T0 for the baseline and T1, T2 and T3 for the years of follow-ups. Variables of interest included demographics: age, gender, education, occupation; measures of functional ability: Activities of Daily Living (ADLs) and Instrumental (IADLs); clinical variables: presence or absence of comorbidity with other pathologies, severity of dementia (Clinical Dementia Rating Scale), behavioral symptoms; and the equivalent scores (ES) of cognitive tests. Logistic regression, random forest and gradient boosting were applied on the baseline data to estimate the MMSE scores (decline of at least >3 points) measured at T3. Patients were divided into multiple splits using different model derivation (training) and validation (test) proportions, and the optimization of the models was carried out through cross validation on the derivation subset only. The models predictive capabilities (balanced accuracy, AUC, AUPCR, F1 score and MCC) were computed on the validation set only. To ensure the robustness of the results, the optimization was repeated 10 times. A SHAP-type analysis was carried out to identify the predictive power of individual variables.ResultsThe model predicted MMSE outcome at T3 with a mean AUC of 0.643. Model interpretability analysis revealed that the global cognitive state progression in AD patients is associated with: low spatial memory (Corsi block-tapping), verbal episodic long-term memory (Babcock's story recall) and working memory (Stroop Color) performances, the presence of hypertension, the absence of hypercholesterolemia, and functional skills inabilities at the IADL scores at baseline.ConclusionThis is the first AI study to predict cognitive trajectories of AD patients using routinely collected clinical data, while at the same time providing explainability of factors contributing to these trajectories. Also, our study used the results of single cognitive tests as a measure of specific cognitive functions allowing for a finer-grained analysis of risk factors with respect to the other studies that have principally used aggregated scores obtained by short neuropsychological batteries. The outcomes of this work can aid prognostic interpretation of the clinical and cognitive variables associated with the initial phase of the disease towards personalized therapies.
ISSN:1663-4365