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Depression and Anxiety Newsletter
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Series 2, Issue 5, 2007
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| USE OF ATYPICAL ANTIDEPRESSANTS IN ELDERLY PATIENTS |
Nancy Byatt, DO, MBA
Harvard University Medical School
Rebecca Lundquist, MD
University of Massachusetts Medical School |
INTRODUCTION
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Late-life major depressive disorder (MDD) is a common disorder that is
associated with severe symptoms and substantial functional impairment.
With an estimated prevalence of 3% in people aged 60 years or more, MDD
has growing health implications for the aging population. In addition,
MDD is often associated with physical disability in this age group as
well as a high mortality rate. Conditions leading to chronic pain, the
presence of comorbid medical illnesses, social isolation, and dysphoria
secondary to life-cycle issues predispose the elderly population to the
development of depression. These factors also point elderly individuals
with depression in the direction of more severe symptoms and a
relatively poor outcome.
While it is a commonly known psychiatric disorder, depression in the
geriatric population is under-recognized and under-treated, leading to
unnecessary impaired social and occupational functioning.1 Studies
suggest that approximately 25% of patients aged 65 years or more who
have a chronic medical illness also experience symptoms of depression.
Evidence supports the increased prevalence of depression in several
specific chronic medical illnesses, including vascular disease, diabetes
mellitus, and arthritis; the relative risk for depression is 2-3 times
higher in these patients than in individuals without these
comorbidities.1 Depression in the geriatric population has also been
reported to be more somatic and less ideational than depression in
younger adults. Elderly people who suffer from comorbid depression and
medical illness have an increased morbidity and mortality.1 Authors have
also noted a brittle response to antidepressant therapy and an increased
risk for chronic depression in the elderly population.2 Safe, effective,
well-tolerated antidepressants are needed for elderly patients with MDD,
especially for those who are also struggling with chronic medical
illness.1
TREATMENT OPTIONS FOR MDD IN THE ELDERLY
The evidence supports the use of selective serotonin reuptake inhibitors (SSRIs)
as first-line therapy for MDD in all age groups. However, in view of their
adverse effect profile and efficacy, atypical antidepressants may also be
considered as a primary treatment option.3 The relatively high comorbid
prevalence of conditions that lead to chronic pain and depression in the elderly
population is of significance, given that a direct relationship between the
intensity of pain and the degree of depression has also been established. In
this subset of geriatric depression, clinicians should consider the use of
serotonin-norepinephrine reuptake inhibitors (SNRIs) such as duloxetine or
venlafaxine in view of the combined effect of this class of medication in
treating both depression and the chronic pain condition.1
Studies also suggest that antidepressant drugs that combine the serotonergic and
noradrenergic mechanisms of action are of comparable efficacy to SSRIs and may
even be modestly more effective in the treatment of MDD.4 Studies also suggest
that treatment with venlafaxine may be effective in geriatric patients with
treatment-resistant MDD and is better tolerated than prescribing additional
medication to augment antidepressant treatment. |
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PHARMACOLOGY AND PHARMACOKINETICS OF ATYPICAL ANTIDEPRESSANTS
SNRIs block the reuptake of both serotonin (5-HT) and norepinephrine with
differing selectivity. They have been shown to be superior to placebo and have
comparable efficacy to the tricyclic antidepressants (TCAs). SNRIs include
venlafaxine and duloxetine and have an adverse effect profile similar to that of
the SSRIs.5 A difference, however, between this class of antidepressants and
other classes is the ability of SNRIs to effectively treat chronic pain
irrespective of whether the pain is related to depression or unrelated.6 In
addition to treating depression, duloxetine may also offer a new treatment for
patients with neuropathic pain and stress urinary incontinence.7 Adverse effects
specific to individual drugs have been documented; venlafaxine has been
associated with hypertension and duloxetine has been associated with
hepatotoxicity.
The dopamine-norepinephrine reuptake inhibitor (DNRI) bupropion primarily blocks
the reuptake of dopamine and norepinephrine with no direct action on the
serotonin system.8 Bupropion has been shown to have efficacy comparable to both
TCAs and SSRIs in the treatment of MDD.5 Bupropion has a lower risk of sexual
dysfunction and weight gain than some other antidepressants and is an effective
alternative or adjunctive treatment for patients whose symptoms do not respond
to SSRIs.8 Compared to SSRIs, treatment with bupropion has the disadvantage of
an increased adverse effect profile that includes headaches, tremors, and
seizures. The risk of seizures decreases at doses less than 450 mg and with
divided dosing.5
The norepinephrine-serotonin modulator mirtazapine enhances the release of
norepinephrine by blocking
α2-adrenergic autoreceptors as well as serotonin
5-HT2A and 5-HT3 receptors and histamine H1 receptors. Its efficacy is similar
to that of TCAs and SSRIs, and it is less likely to cause sexual adverse
effects. Mirtazapine has been associated with weight gain and sedation, which
can be helpful for patients who are also experiencing decreased appetite and
insomnia.9
Serotonin modulators, which include nefazodone and trazodone, block the 5-HT2A
serotonin receptor and serotonin reuptake and have an antidepressant efficacy
similar to that of SSRIs. Nefazodone and trazodone and are less commonly used to
treat depression because of their adverse-effect profiles of hepatoxicity and
sedation, respectively. Trazodone is mainly used in clinical practice for its
sedative properties separate from the treatment of depression.5 |
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SPECIAL CONSIDERATIONS WHEN PRESCRIBING ATYPICAL ANTIDEPRESSANTS TO ELDERLY PATIENTS
The presence of
high levels of pain in elderly patients may diminish the degree of response for
the comorbid symptoms of depression for any given antidepressant therapy. The
detection, diagnosis, and management of chronic pain should routinely include
the identification and treatment of coexisting medical conditions that may
contribute to or complicate late-life depression. Both the depression and the
comorbid medical condition that is contributing to the depression should be
treated from the outset.3
When prescribing an
antidepressant to an elderly patient, the initial dose of the agent must be
determined by individual symptom response, known adverse effect profile,
drug-drug interactions, and any comorbid medical and psychiatric conditions. The
initial dose selected may be smaller than that prescribed to younger patients
because of age-related physiological changes such as impaired hepatic and renal
elimination that can result not only in higher serum concentrations of the drug
for a given dose but also in a higher likelihood of adverse effects. As a general
rule of thumb, clinicians should “start low and go slow” when prescribing
antidepressants to elderly patients.10
While venlafaxine may be
effective and be associated with fewer drug-drug interactions and a generally
favorable adverse effect profile, it is associated with some undesirable
cardiovascular effects, such as hypertension, orthostatic hypertension, and
new-onset tachycardia or palpitations. Systematic monitoring of cardiovascular
parameters is strongly recommended in elderly patients, especially those who are
taking more than 150 mg of venlafaxine per day.11
Mirtazapine, like SSRIs, has
been reported to uncommonly cause hyponatremia. While this adverse effect is
uncommon, it should be considered in any elderly patient with altered mental
status who has recently started to take mirtazapine.12
The issue of drug-drug interactions is of
particular relevance for geriatric patients because of the increased likelihood
of polypharmacy for comorbid illnesses. Polypharmacy may lead not only to
notable adverse effects as a result of the interaction of medications but also
to an increased risk of known adverse effects from the prescribed
antidepressant. The antidepressants with the least potential for altering drug
metabolism are some of the SSRIs, such as citalopram, and the selected atypical
antidepressants, such as venlafaxine, duloxetine, and mirtazapine.13 |
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REFERENCES
- Wise TN, Wiltse CG, Iosifescu DV, et al. The safety and tolerability of
duloxetine in depressed elderly outpatients with and without medical
comorbidity. Int J Clin Pract. 2007:61(8);1283-93.
- Meltzer CC, Price JC, Mathis CA,
et al. Serotonin 1A receptor binding and treatment response in late-life
depression. Neuropsychopharmacology. 2004;29(12):2258-65.
- Alexopoulos GS,
Katz GS, Reynolds CF, et al. The expert consensus guidelines series.
Pharmacotherapy of depressive disorders in older patients. Postgrad Med.
2001;Oct:1-86.
- Papakostas GI, Thase ME, Fava M,
et al. Are antidepressant drugs that combine serotonergic and noradrenergic
mechanisms of action more effective than the SSRIs in treating major
depressive disorder? A meta-analysis of studies of newer agents.
Biol Psychiatry. 2007;[Epub ahead of print].
- American Psychiatric
Association. Practice guideline for the treatment of patients with major
depressive disorder (revision). Am J Psychiatry. 2000;157(4 Suppl):1-45.
- Stahl SM, Grady MM. Moret C, Briley M. SNRIs: their
pharmacology, clinical efficacy, and tolerability in comparison with other
classes of antidepressants. CNS Spectr. 2005;10(9):732-47.
- Westanmo AD, Gayken JM, Haight R. Duloxetine: a
balanced and selective norepinephrine- and serotonin-reuptake inhibitor.
Am J Health Syst Pharm. 2005:62;2481-90.
- Papakostas GI. Dopaminergic-based
pharmacotherapies for depression. Eur Neuropsychopharmacol.
2006:16(6);391-402.
- Mann JJ. The medical management
of depression. N Engl J Med. 2005;353(17):1819-34.
- Antai-Otong D. Poststroke
depression: psychopharmacological considerations. Perspect Psychiatr
Care. 2004:40(4);167-70.
- Johnson EM, Whyte E, Mulsant BH,
et al. Cardiovascular changes associated with venlafaxine in the treatment
of late-life depression. Am J Geriatr Psychiatry. 2006:14(9);796-802.
- Ladino M, Guardiola VD, Paniagua
M. Mirtazapine-induced hyponatremia in an elderly hospice patient. J
Palliat Med. 2006:9(2);258-60.
- Levy RH, Collins C. Risk and
predictability of drug interactions in the elderly. Int Rev Neurobiol.
2007:81;235-51.
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Nancy Byatt, DO, MBA
Psychosomatic Medicine Fellow
Brigham and Women's Hospital
Harvard University Medical School |
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Rebecca Lundquist, MD
Assistant Professor
Psychiatry
University of Massachusetts Medical School
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