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Summary
February 2007, Vol. 8, No. 2, Pages 203-214
, DOI 10.1517/14656566.8.2.203
Memantine in the treatment of mild-to-moderate Alzheimer’s diseaseKelly M Cosman1University of Rochester School of Medicine, Alzheimer’s Disease Care Research and Education Program (AD-CARE), Monroe Community Hospital, 435 East Henrietta Road, Rochester, NY 14620, USA. Kelly_Cosman@urmc.rochester.edu 2University of Rochester School of Medicine, Psychiatry Department, 300 Crittenden Boulevard, Rochester, NY 14642, USA. Lisa_Boyle@urmc.rochester.edu 3University of Rochester School of Medicine, Alzheimer’s Disease Care Research and Education Programme (AD-CARE), Monroe Community Hospital, 435 East Henrietta Road, Rochester, NY 14620, USA. Anton_Porsteinsson@urmc.rochester.edu †  Author for correspondenceMemantine is the first and only medication that has been approved by European, US and Canadian regulatory agencies for the treatment of moderate-to-severe Alzheimer’s disease (AD). It is an NMDA receptor antagonist that works to prevent excitotoxicity and cell death, which are mediated by the excessive influx of calcium during a sustained release of glutamate. Preclinical studies of memantine reveal that it has the potential to improve memory and learning processes after impairment has occurred, as well as to prevent further neuronal damage. Although memantine has been considered for the treatment of earlier AD, it has not yet been approved for this. Randomized controlled trials of memantine in the treatment of mild-to-moderate AD have demonstrated small treatment effects in measures of cognition, global assessment and behavior favoring the use of memantine. However, the differences between treatment groups were not consistently significant. Two ongoing long-term trials are further investigating the efficacy of memantine in the treatment of mild-to-moderate AD. Forward Links to Citing ArticlesJared  K. Nelson, SidselU. Frølund, DennisB. Tikhonov, AndersS. Kristensen, Kristian Strømgaard. (2009) Synthesis and Biological Activity of Argiotoxin636 and Analogues: Selective Antagonists for Ionotropic Glutamate Receptors. Angewandte Chemie International Edition 48:17, 3087-3091Online publication date: 14-May-2009. CrossRef Jared K. Nelson, SidselU. Frølund, DennisB. Tikhonov, AndersS. Kristensen, Kristian Strømgaard. (2009) Synthesis and Biological Activity of Argiotoxin636 and Analogues: Selective Antagonists for Ionotropic Glutamate Receptors. Angewandte Chemie 121:17, 3133-3137Online publication date: 14-May-2009. CrossRef Lêda S. Garcia, Clarissa M. Comim, Samira S. Valvassori, Gislaine Z. Réus, Ana Cristina Andreazza, Laura Stertz, Gabriel R. Fries, Elaine Cristina Gavioli, Flavio Kapczinski, João Quevedo. (2009) Chronic Administration of Ketamine Elicits Antidepressant-Like Effects in Rats without Affecting Hippocampal Brain-Derived Neurotrophic Factor Protein Levels. Basic & Clinical Pharmacology & Toxicology 103:6, 502-506 Online publication date: 1-Jan-2009. CrossRef Emily O. Dumas, Gary M. Pollack. (2008) Opioid Tolerance Development: A Pharmacokinetic/Pharmacodynamic Perspective. The AAPS Journal Online publication date: 7-Dec-2008. CrossRef (2007) Current awareness in geriatric psychiatry. International Journal of Geriatric Psychiatry 22:10, 1055-1062 Online publication date: 1-Nov-2007. CrossRef V A Campbell, A Gowran. (2007) Alzheimer's disease; taking the edge off with cannabinoids?. British Journal of Pharmacology CrossRef |
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