A brief review of the pharmacologic and therapeutic aspects of memantine in Alzheimer’s disease

Frederick Schmitt

‌^†¹, Melody Ryan

‌² & Gregory Cooper

‌³^,⁴

¹University of Kentucky, Sanders-Brown Center on Aging, and Department of Neurology, and Departments of Psychiatry, Psychology, and Behavioural Sciences, 800 S. Limestone Street, Lexington, KY 40536-0230, USA. fascom@email.uky.edu

²University of Kentucky, Department of Neurology, and Department of Pharmacy Practice and Science, 800 S. Limestone Street, Lexington, KY 40536-0230, USA

³University of Kentucky, Sanders-Brown Center on Aging, and Department of Neurology, 800 S. Limestone Street, Lexington, KY 40536-0230, USA

⁴Lexington Clinic, Division of Neurology, Lexington, KY, USA

†

Author for correspondence

The past decade has seen an increase in therapeutic options for Alzheimer’s disease (AD) that target neurotransmitters, such as acetylcholine, and research continues to target abnormal proteins in the AD brain. Recently, glutamate excitotoxicity has also become a target for AD treatment with the advent of memantine. Clinical trial data reviewed for memantine show good tolerability, low side-effect profiles and a positive therapeutic impact in moderate-to-severe AD, both as monotherapy and in conjunction with donepezil. However, additional data suggest variable benefits in the mild stages of AD. Furthermore, published reports support reduced dosing in patients with significant renal disease. However, the opportunity to target a second mechanism in the treatment of AD, thereby providing added symptomatic benefit, appears to be a useful consideration for clinicians who treat this devastating neurodegenerative disorder.

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Forward Links to Citing Articles

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