Plasma MCP-1 and changes on cognitive function in community-dwelling older adults

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Sánchez-Sánchez, Juan Luis | Giudici, Kelly, V | Gillette-Guyonnet, Sophie | Delrieu, Julien | Li, Yan | Bateman, Randall, J | Parini, Angelo | Vellas, Bruno | Barreto de Souto, Philipe | Carrié, Isabelle | Brigitte, Lauréane | Faisant, Catherine | Lala, Françoise | Villars, Hélène | Combrouze, Emeline | Badufle, Carole | Zueras, Audrey | Andrieu, Sandrine | Cantet, Christelle | Morin, Christophe | van Kan, Gabor, Abellan | Dupuy, Charlotte | Rolland, Yves | Caillaud, Céline | Ousset, Pierre-Jean | Willis, Sherry | Belleville, Sylvie | Gilbert, Brigitte | Fontaine, Francine | Dartigues, Jean-François | Marcet, Isabelle | Delva, Fleur | Foubert, Alexandra | Cerda, Sandrine | Costes, Corinne | Rouaud, Olivier | Manckoundia, Patrick | Quipourt, Valérie | Marilier, Sophie | Franon, Evelyne | Bories, Lawrence | Pader, Marie-Laure | Basset, Marie-France | Lapoujade, Bruno | Faure, Valérie | Tong, Michael, Li Yung | Malick-Loiseau, Christine | Cazaban-Campistron, Evelyne | Desclaux, Françoise | Blatge, Colette | Dantoine, Thierry | Laubarie-Mouret, Cécile | Saulnier, Isabelle | Clément, Jean-Pierre | Picat, Marie-Agnès | Bernard-Bourzeix, Laurence | Willebois, Stéphanie | Désormais, Iléana | Cardinaud, Noëlle | Bonnefoy, Marc | Livet, Pierre | Rebaudet, Pascale | Gédéon, Claire | Burdet, Catherine | Terracol, Flavien | Pesce, Alain | Roth, Stéphanie | Chaillou, Sylvie | Louchart, Sandrine | Sudres, Kristel | Lebrun, Nicolas | Barro-Belaygues, Nadège | Touchon, Jacques | Bennys, Karim | Gabelle, Audrey | Romano, Aurélia | Touati, Lynda | Marelli, Cécilia | Pays, Cécile | Robert, Philippe | Le Duff, Franck | Gervais, Claire | Gonfrier, Sébastien | Gasnier, Yannick | Bordes, Serge | Begorre, Danièle | Carpuat, Christian | Khales, Khaled | Lefebvre, Jean-François | El Idrissi, Samira, Misbah | Skolil, Pierre | Salles, Jean-Pierre | Dufouil, Carole | Lehéricy, Stéphane | Chupin, Marie | Mangin, Jean-François | Bouhayia, Ali | Allard, Michèle | Ricolfi, Frédéric | Dubois, Dominique | Martel, Marie, Paule Bonceour | Cotton, François | Bonafé, Alain | Chanalet, Stéphane | Hugon, Françoise | Bonneville, Fabrice | Cognard, Christophe | Chollet, François | Payoux, Pierre | Voisin, Thierry | Peiffer, Sophie | Hitzel, Anne | Zanca, Michel | Monteil, Jacques | Darcourt, Jacques | Molinier, Laurent | Derumeaux, Hélène | Costa, Nadège | Perret, Bertrand | Vinel, Claire | Caspar-Bauguil, Sylvie | Olivier-Abbal, Pascale | Coley, Nicola

Edité par CCSD ; BioMed Central -

International audience. Background: Monocyte Chemoattractant Protein-1 (MCP-1), a glial-derived chemokine, mediates neuroinflammation and may regulate memory outcomes among older adults. We aimed to explore the associations of plasma MCP-1 levels (alone and in combination with β-amyloid deposition-Aβ42/40) with overall and domain-specific cognitive evolution among older adults.Methods: Secondary analyses including 1097 subjects (mean age = 75.3 years ± 4.4; 63.8% women) from the Multidomain Alzheimer Preventive Trial (MAPT). MCP-1 (higher is worse) and Aβ42/40 (lower is worse) were measured in plasma collected at year 1. MCP-1 in continuous and as a dichotomy (values in the highest quartile (MCP-1+)) were used, as well as a dichotomy of Aβ42/40. Outcomes were measured annually over 4 years and included the following: cognitive composite z-score (CCS), the Mini-Mental State Examination (MMSE), and Clinical Dementia Rating (CDR) sum of boxes (overall cognitive function); composite executive function z-score, composite attention z-score, Free and Cued Selective Reminding Test (FCSRT - memory).Results: Plasma MCP-1 as a continuous variable was associated with the worsening of episodic memory over 4 years of follow-up, specifically in measures of free and cued delayed recall. MCP-1+ was associated with worse evolution in the CCS (4-year between-group difference: β = -0.14, 95%CI = -0.26, -0.02) and the CDR sum of boxes (2-year: β = 0.19, 95%CI = 0.06, 0.32). In domain-specific analyses, MCP-1+ was associated with declines in the FCSRT delayed recall sub-domains. In the presence of low Aβ42/40, MCP-1+ was not associated with greater declines in cognitive functions. The interaction with continuous biomarker values Aβ42/40× MCP-1 × time was significant in models with CDR sum of boxes and FCSRT DTR as dependent variables.Conclusions: Baseline plasma MCP-1 levels were associated with longitudinal declines in overall cognitive and episodic memory performance in older adults over a 4-year follow-up. How plasma MCP-1 interacts with Aβ42/40 to determine cognitive decline at different stages of cognitive decline/dementia should be clarified by further research. The MCP-1 association on cognitive decline was strongest in those with amyloid plaques, as measured by blood plasma Aβ42/40.

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