Abstract
Dementia represents a global health challenge due to the increase in elderly population worldwide. In addition to memory loss, dementia often results in severe behavioral and psychological changes where pharmacological treatments might be considered in addition to nonpharmacological strategies for optimal symptomatic control. Risperidone, the second oldest atypical antipsychotic, has been widely used off-label to treat behavioral and psychological symptoms of dementia (BPSD), including agitation, aggression, and psychosis. Several studies have indicated that risperidone offers a modest and statistically significant effectiveness in the clinical setting. However, in the past decade, safety concerns emerged due to increased risk for cerebrovascular adverse events and death following the use of risperidone in the elderly population. Clinical guidelines suggest that, in severe dementia where an older adult is threatening to harm himself or others, pharmacological treatments might be considered when nonpharmacological treatments fail. Risperidone was approved for BPSD in some countries (Australia, Canada, United Kingdom and New Zealand) but not in the United States. This article reviews risperidone’s pharmacological activity, clinical effectiveness and safety, marketing approval, and off-label use in BPSD.
Highlights
More than 40 million people live with dementia worldwide, and this number is projected to triple by 2050 (Prince et al, 2015)
CVAE; There was a significant increase in the et al, 2011 MA atypical antipsychotic vs significantly improve global scores risk of CVAE for risperidone compared with medications for use in conditions Placebo compared with placebo (SMD, 0.19; 95% placebo (OR, 3.12; 95% CI, 1.32, 8.21; 4 lacking approval for labeling and CI, 0, 0.38; 6 studies)
CVAE; There was a significant increase in the Shamliyan, MA atypical antipsychotics for vs Behave-AD; risperidone did not significantly risk of CVAE for risperidone compared with people with dementia
Summary
More than 40 million people live with dementia worldwide, and this number is projected to triple by 2050 (Prince et al, 2015). It occurs more commonly in persons 65 or older, and with the growing elderly population in developed countries, dementia represents a global health challenge (Plassman et al, 2007; Livingston et al, 2017). Among all the atypical antipsychotics, risperidone has the most clinical trial-related evidence to support its use in BPSD (Lee et al, 2006). We will focus on the role of risperidone, one of the oldest and most widely used atypical antipsychotics in the management of BPSD. We will first review risperidone’s pharmacological activity, secondly, we will explore the clinical evidence behind its use in BPSD and we will examine its worldwide regulatory approval and off-label use in BPSD
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