Cognitive impact of multidomain intervention and omega 3 according to blood A[beta]42/40 ratio: a subgroup analysis from the randomized MAPT trial

Cognitive impact of multidomain intervention and omega 3 according to blood A[beta]42/40 ratio: a subgroup analysis from the randomized MAPT trial

Background In MAPT (Multidomain Alzheimer Preventive Trial), a cognitive effect of multidomain intervention (MI) was showed in non-demented subjects with positive amyloid PET. However, screening eligible patients for multidomain intervention by PET is difficult to generalize in real-world settings....

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Veröffentlicht in:Alzheimer's research & therapy 2023-10, Vol.15 (1)
Hauptverfasser: Begorre, Danièle, Morin, Christophe, Burdet, Catherine, Chaillou, Sylvie, Willebois, Stéphanie, Livet, Pierre, Faure, Valérie, Ovod, Vitaliy, Quipourt, Valérie, Bollinger, James, Tong, Michael Li Yung, Cazaban-Campistron, Evelyne, Robert, Philippe, Delrieu, Julien, Khales, Khaled, Roth, Stéphanie, Van Kan, Gabor Abellan, Clément, Jean-Pierre, Cardinaud, Noëlle, Romano, Aurélia, Rolland, Yves, Brigitte, Lauréane, Bateman, Randall, Cantet, Christelle, Faisant, Catherine, Saulnier, Isabelle, Touchon, Jacques, Desclaux, Françoise, Bennys, Karim, Villars, Hélène, Manckoundia, Patrick, Lala, Françoise, Carrié, Isabelle, Andrieu, Sandrine, Costes, Corinne, Bernard-Bourzeix, Laurence, Laubarie-Mouret, Cécile, Bonnefoy, Marc, Gervais, Claire, Gilbert, Brigitte, Rouaud, Olivier, Louchart, Sandrine, Coley, Nicola, Combrouze, Emeline, Pesce, Alain, Dupuy, Charlotte, Basset, Marie-France, Rebaudet, Pascale, Ousset, Pierre-Jean, Carpuat, Christian, Désormais, Iléana, Dartigues, Jean-François, Marelli, Cécilia, Zueras, Audrey, Lebrun, Nicolas, Franon, Evelyne, Barro-Belaygues, Nadège, Skolil, Pierre, Salles, Jean-Pierre, Willis, Sherry, Gonfrier, Sébastien, Foubert, Alexandra, Lapoujade, Bruno, Sudres, Kristel, Gabelle, Audrey, Le Duff, Franck, Marilier, Sophie, Blatge, Colette, Dantoine, Thierry, Bordes, Serge, Gasnier, Yannick, Lefebvre, Jean-François, Guyonnet, Sophie, Marcet, Isabelle, Delva, Fleur, Terracol, Flavien, Picat, Marie-Agnès, Pays, Cécile, Li, Yan, Fontaine, Francine, Touati, Lynda, Caillaud, Céline, Pader, Marie-Laure, Gédéon, Claire, El Idrissi, Samira Misbah, Vellas, Bruno, Cerda, Sandrine, Malick-Loiseau, Christine, Badufle, Carole, Belleville, Sylvie, Bories, Lawrence
Format: Artikel
Sprache:eng
Schlagworte:
Alzheimer's disease
Analysis
Biological markers
Care and treatment
Clinical trials
Diagnosis
Dosage and administration
Ethylenediaminetetraacetic acid
Mass spectrometry
Medical colleges
Neurologic manifestations of general diseases
Omega-3 fatty acids
Prevention
Risk factors
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Zusammenfassung:Background In MAPT (Multidomain Alzheimer Preventive Trial), a cognitive effect of multidomain intervention (MI) was showed in non-demented subjects with positive amyloid PET. However, screening eligible patients for multidomain intervention by PET is difficult to generalize in real-world settings. Methods MAPT study was a 3-year, randomized, placebo-controlled trial followed by a 2-year observational and optional extension. All participants were non-demented and randomly assigned (1:1:1:1) to the MI plus omega 3, MI plus placebo, omega 3 alone, or placebo alone group. The objectives were to assess the cognitive effect of MAPT interventions (omega 3 supplementation, MI, combined intervention) in non-demented subjects according to amyloid blood status at 12, 36, and 60 months. In this subgroup analysis (n = 483), amyloid status was defined by plasma A[beta]42/40 ratio (cutoff [less than or equal to] 0.0107). The primary outcome measure was the change in cognitive composite score after a 1, 3, and 5-year clinical follow-up. Results The intention-to-treat (ITT) population included 483 subjects (161 positive and 322 negative amyloid participants based on plasma A[beta]42/40 ratio). In the positive amyloid ITT population, we showed a positive effect of MI plus omega 3 on the change in composite cognitive score in 12 (raw p = .0350, 0.01917, 95% CI = [0.0136 to 0.3699]) and 36 months (raw p = .0357, 0.2818, 95% CI = [0.0190 to 0.5446]). After correction of multiple comparisons and adjustments, these differences were not significant (adjusted p = .1144 and .0690). In the per-protocol positive amyloid group (n = 154), we observed a significant difference between the combined intervention and placebo groups at 12 (p = .0313, 0.2424, 0.0571 to 0.4276) and 36 months (p = .0195, 0.3747, 0.1055 to 0.6439) persisting after adjustment. In the ITT and per-protocol analyses, no cognitive effect was observed in the positive and negative amyloid group at 60-month visit. Conclusions These findings suggest a benefit of MI plus omega 3 in positive blood amyloid subjects. This promising trend needs to be confirmed before using blood biomarkers for screening in preventive trials. Trial registration ClinicalTrials.gov Identifier: NCT01513252. Keywords: Clinical trial, Alzheimer's disease, Amyloid blood biomarker, Prevention
ISSN:1758-9193
1758-9193
DOI:10.1186/s13195-023-01325-3