Lithium as a Treatment for Alzheimer’s Disease: The Systems Pharmacology Perspective
Article type: Review Article
Authors: Hampel, Haralda; * | Lista, Simonea; b; c | Mango, Dalilad | Nisticò, Robertd; e | Perry, Georgef | Avila, Jesusg; h | Hernandez, Felixg; h | Geerts, Hugoi | Vergallo, Andreaa; b; c; * | Alzheimer Precision Medicine Initiative (APMI)1; 2
Collaborators: AFSHAR, Mohammad | AGUILAR, Lisi Flores | AKMAN-ANDERSON, Leyla | ARENAS, Joaquín | AVILA, Jesus | BABILONI, Claudio | BALDACCI, Filippo | BATRLA, Richard | BENDA, Norbert | BLACK, Keith L. | BOKDE, Arun L.W. | BONUCCELLI, Ubaldo | BROICH, Karl | CACCIOLA, Francesco | CARACI, Filippo | CASTRILLO†, Juan | CAVEDO, Enrica | CERAVOLO, Roberto | CHIESA, Patrizia A. | CORVOL, Jean-Christophe | CUELLO, Augusto Claudio | CUMMINGS, Jeffrey L. | DEPYPERE, Herman | DUBOIS, Bruno | DUGGENTO, Andrea | EMANUELE, Enzo | ESCOTT-PRICE, Valentina | FEDEROFF, Howard | FERRETTI, Maria Teresa | FIANDACA, Massimo | FRANK, Richard A. | GARACI, Francesco | GEERTS, Hugo | GIORGI, Filippo S. | GOETZL, Edward J. | GRAZIANI, Manuela | HABERKAMP, Marion | HABERT, Marie-Odile | HAMPEL, Harald | HERHOLZ, Karl | HERNANDEZ, Felix | KAPOGIANNIS, Dimitrios | KARRAN, Eric | KIDDLE, Steven J. | KIM, Seung H. | KORONYO, Yosef | KORONYO-HAMAOUI, Maya | LANGEVIN, Todd | LEHÉRICY, Stéphane | LUCÍA, Alejandro | LISTA, Simone | LORENCEAU, Jean | MANGO, Dalila | MAPSTONE, Mark | NERI, Christian | NISTICÓ, Robert | O’BRYANT, Sid E. | PALERMO, Giovanni | PERRY, George | RITCHIE, Craig | ROSSI, Simone | SAIDI, Amira | SANTARNECCHI, Emiliano | SCHNEIDER, Lon S. | SPORNS, Olaf | TOSCHI, Nicola | VERDOONER, Steven R. | VERGALLO, Andrea | VILLAIN, Nicolas | WELIKOVITCH, Lindsay A. | WOODCOCK, Janet | YOUNESI, Erfan
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Correspondence: [*] Correspondence to: Andrea Vergallo, MD & Harald Hampel, MD, PhD, AXA Research Fund & Sorbonne University Chair, Sorbonne University, Department of Neurology, Institute of Memory and Alzheimer’s Disease (IM2A), Brain & Spine Institute (ICM), François Lhermitte Building, Pitié-Salpêtrière Hospital, 47 Boulevard de l’hôpital, 75651 Paris CEDEX 13, France. E-mail: [email protected] (A. Vergallo), [email protected] (H. Hampel).
Note: [1] Sorbonne University Clinical Research Group (GRC n°21), “Alzheimer Precision Medicine (APM)”, Établissements Publics á caractère Scientifique et Technologique (E.P.S.T.)
Note: [2] Alzheimer Precision Medicine Initiative (APMI), https://www.apmiscience.com/
Abstract: Systems pharmacology is a novel framework for drug research that models traditional and innovative pharmacological parameters and provides the overall efficacy and safety profile of a drug across body systems and complex, non-linear, molecular interactions. Lithium chloride, a pharmacological compound approved for the therapy of psychiatric disorders, represents a poorly explored compound for the treatment of Alzheimer’s disease (AD). Lithium has been shown to reduce downstream effects associated with the aberrant overactivation of certain molecular pathways, such as glycogen synthase kinase 3 subunit β (GSK3-β)-related pathways, involved in AD-related pathophysiology. It seems that overactivation and overexpression of GSK3-β lead to an impairment of long-term potentiation and amyloid-β induced neurotoxicity that can be normalized using lithium. Moreover, a growing body of evidence has demonstrated that lithium’s GSK3-β inhibitory effect prevents tau phosphorylation in mouse models of tauopathies. Clinical data have been inconclusive, partly due to methodological limitations. The lack of studies exploring the dynamics of protein misfolding in AD and investigating the specific tau-isoforms appearing prior to the accumulation of neurofibrillary tangles calls for new and optimized clinical trials. Advanced computer modeling based on a formal implementation of quantitative parameters and basic enzymatic insights into a mechanism-based model would present a good start to tackle these non-linear interactions. This innovative approach will pave the way for developing “molecularly” biomarker-guided targeted therapies, i.e., treatments specifically adapted (“tailored”) to the individual, consistently with the primary objectives and key conceptual points of precision medicine and precision pharmacology.
Keywords: Alzheimer’s disease, GSK3, lithium, neurotoxicity, precision medicine, post-translational modification, systems pharmacology, tau
DOI: 10.3233/JAD-190197
Journal: Journal of Alzheimer's Disease, vol. 69, no. 3, pp. 615-629, 2019