Major Depressive Disorder Clinical Trial
Official title:
Effects of Combined Memantine (Namenda) Plus Escitalopram (Lexapro) Treatment in Elderly Depressed Patients With Cognitive Impairment
Alzheimer's disease (AD), the most common dementing disorder of later life, is a major cause
of disability and death in the elderly. Although a number of theoretical causes exist, the
etiology of AD is still unknown. Consequently, the focus of treatments has been palliative,
designed to ameliorate AD symptoms. Recent efforts, however, have revealed some surprising
data suggesting that cholinesterase inhibitors (AchEIs), used over the last decade, and
recently released memantine (an N-methyl-D-aspartate (NMDA) receptor antagonist), may confer
protection to neurons. Thus, they may offer a slowing of cognitive decline and/or
improvement in behavioral symptoms associated with memory impairment.
Over the last decade, it has been well documented that mild cognitive impairment (MCI)
increases the risk of conversion to AD and that coincident depression and MCI (Dep-MCI)
further increases the risk 2 to 3 fold. The primary focus of this line of investigation is
to treat the very high risk to dement patient population with Dep-MCI, before they develop
AD, in the hopes of delaying AD onset.
Memantine had not been studied in DEP-MCI patients. Since treatment of these patients with
combined antidepressant and AChEIs has been associated with cognitive improvement in pilot
studies, we explore whether treatment of DEP-MCI with memantine in addition to
antidepressant treatment would benefit cognitive performance and lead to a low rate of
conversion to dementia. We evaluate the cognitive and antidepressant benefit of combined
open-label es-citalopram and memantine treatment over 48 weeks in a DEP-CI sample.
The study is conducted in a sample of 35 elderly (50-90 years old) outpatients who meet
study inclusion criteria for depression (DEP) (DSM-IV criteria for major depression,
dysthymic disorder, or depression NOS) and mild cognitive impairment (MCI; e.g.
operationally defined as between "normal" and "dementia"), i.e., Dep-MCI. The research plan
includes: i) Obtaining a baseline psychiatric and neuropsychological test profile, ii) If
currently on an ineffective antidepressant, having a one week washout (3 weeks for
fluoxetine), iii) A treatment trial beginning with a two-week es-citalopram lead-in period.
At two weeks, memantine (Namenda) is added starting at 5 mg/day and increased until the
maximum dose of 20 mg/day is reached by six weeks. The study psychiatrist administers: the
24-item Hamilton Depression Rating Scale (HAM-D); the Clinical Global Impression (CGI, 1-7
scale) initial severity and subsequent change ratings separately for depression, cognition,
and overall clinical status; the Treatment Emergent Symptom Scale (TESS) for somatic side
effects. A trained technician administers the neuropsychological battery at baseline, 12, 24
and 48 weeks. If the patient is an antidepressant non-responder during the first 12-weeks,
the es-citalopram is changed to an alternative antidepressant, as clinically indicated by
the treating psychiatrist. The patient remains on the memantine for the entire 48-weeks,
irrespective of antidepressant response.
This will tell us about the efficacy and tolerability of es-citalopram+memantine on both
cognitive and depressive symptoms in Dep-MCI patients and will potentially have broader
public health implications because Dep-MCI is a wide-spread clinical problem where
management needs to be improved.
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Endpoint Classification: Efficacy Study, Intervention Model: Single Group Assignment, Masking: Open Label, Primary Purpose: Treatment
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