Patients receiving
antidepressant monotherapy may be partially or totally
resistant to treatment in 10 to 30 percent of cases. In patients who have
experienced only partial treatment results, the clinician should first
consider optimizing antidepressant dosage or lengthening therapy.
Antidepressant drug substitution should generally be reserved for use in
patients who haven't responded at all (nonresponders). Combining two or more
antidepressants is generally not recommended, as this approach may obscure
adequate monotherapy evaluation and lead to significant adverse effects or
drug-drug interactions. Use of electroconvulsive therapy is recommended in
patients with psychotic and severe refractory depression. Augmentation
therapy is often efficacious in patients who exhibit a partial
antidepressant response. Lithium and thyroid hormone have been the most
extensively studied augmentative agents but, more recently, pindolol and
buspirone have also been used for this purpose.
Partial response and nonresponse to antidepressant medications are common
problems in patients with depression. Between 10 and 30 percent of depressed
patients taking an antidepressant are partially or totally resistant to the
treatment. Recurrence of depression while still taking medication (i.e.,
breakthrough) can also occur.
Several factors may contribute to treatment failure, including undiagnosed or
misdiagnosed medical conditions such as hypothyroidism and anemia. Therefore,
the patient who does not respond or only partially responds to an antidepressant
should first be reassessed to make sure the original diagnosis of depression was
correct. Also, nonpsychiatric drugs such as methyldopa (Aldomet), beta blockers
and reserpine (Serpasil) can cause or exacerbate depression. In addition,
comorbid disorders (e.g.,
eating disorders,
substance abuse or dependence) may
affect treatment response. Psychotic depression,
bipolar depression and atypical
depression are depressive subtypes that may require concurrent pharmacotherapy
such as antipsychotic or augmentative psychotherapy. Finally, adverse effects
and poor compliance may be additional obstacles to successful treatment.
Strategies for Partial Response and Nonresponse
Five strategies for treating partial response or nonresponse to
antidepressant therapy are optimization,
drug substitution,
combination therapy,
electroconvulsive therapy and augmentation therapy.
Optimization
Prescribing antidepressant medication in dosages that are too low and for
lengths of time that are too short are common causes of treatment failure. In a
study conducted in a managed care environment, only 11 percent of patients
requiring antidepressant therapy received either an adequate therapeutic dosage
or an adequate duration of therapy. Inadequate antidepressant dosage and
duration are particularly prevalent in elderly patients.
|
Between 10 and 30 percent of
patients with depression are partially or totally resistant to
antidepressant therapy. |
When a patient's history suggests inadequate therapy, the clinician should
maximize the dosage or duration of therapy. Some depressed patients who are resistant to
treatment may benefit from antidepressant dosages that are higher than the usual
recommendations.
An adequate duration for a trial of antidepressant therapy has been defined
by some clinicians as four to six weeks. Others assert that a minimum of six
weeks is necessary. If the patient exhibits a partial response during this
initial period, another four to six weeks of treatment should be added. Thus, a
total of 10 to 12 weeks may be required in some cases to elicit a full
antidepressant response.
Drug Substitution
"Nonresponders" are most likely to benefit from drug substitution. A change
from one antidepressant to another in the same class has not produced impressive
response rates among depressed patients. However, uncontrolled studies suggest
that switching to an antidepressant with a different mechanism of action is
often associated with a better response rate. Uncontrolled trials suggest that
switching from a tricyclic antidepressant to an alternative antidepressant class
may result in a 50 to 60 percent positive response rate.
Combination Therapy
| TABLE 1
Pros and Cons of Combination/ Augmentation Strategies
Pros
-Strategy builds on therapeutic gains
-Addition of second compound is generally well tolerated
-More rapid onset of antidepressant effects
-Response rate comparable or superior to drug substitution
Cons
-Polypharmacy and the potential for increasing drug interaction
-Reduced compliance
-Increased adverse effects |
Combination therapy involves the addition of a second antidepressant agent to
the therapeutic regimen. Concurrent administration of two or more antidepressant
agents (e.g., adding trazodone [Desyrel], desipramine [Norpramine] or bupropion
[Wellbutrin] to fluoxetine) may result in a different therapeutic response than
that produced by use of either drug alone. However, no double-blind,
placebo-controlled studies recommend the usefulness of this practice. In
addition, this approach does not allow for adequate evaluation of monotherapy
and may lead to significant adverse effects or drug-drug interactions (Table
1).
Electroconvulsive therapy is still the most effective treatment for psychotic
depression and severe refractory depression. The clinician should not hesitate
to recommend it and should reassure patients as to its appropriate and safe use
under medically monitored conditions.
Augmentation Therapy
Augmentation therapy involves adding a second agent, but one that is not
routinely regarded as an antidepressant, to the therapeutic regimen when there
is only a partial response to the antidepressant agent.1,6 Four agents
frequently used in augmentation therapy are lithium, thyroid hormone, the beta
blocker pindolol (Visken) and buspirone (Buspar). It is helpful to review the
neurotransmitter serotonin, the 5-HT receptor and the mechanism for
antidepressant actions as they relate to the 5-HT1A receptor to
understand the rationale for augmentation therapy.
Serotonin. Serotonin plays an important role in sleep, appetite,
memory and mood. Serotonin release is inhibited or enhanced by the activity of
the 5-HT1A receptor. Stimulation of the presynaptic somatodendritic
5-HT1A receptor by high levels of synaptic serotonin results in a
negative feedback mechanism that inhibits further serotonin synthesis and
release. Depression is associated with a relative lack of serotonin and
norepinephrine in the synaptic cleft and, thus, a lack of normal responsiveness
of the postsynaptic 5-HT1A receptors to stimulate the release of more
serotonin. Although this description conveys a simplistic notion of a complex
process, the serotonin hypothesis of depression has recently been expanded by
the discovery that the true antidepressant effect (hence the four-to-six week
delay in obtaining clinical improvement) may be due to the "down regulation" of
central beta-adrenergic receptors by the antidepressant agent.
Lithium. Lithium has been the most widely used and extensively studied
augmentation agent. It apparently enhances serotonin transmission by reducing
the activity of post-synaptic serotonin or 5-HT receptors. This, in turn,
reduces the negative feedback to serotonin-releasing cells and thereby increases
serotonin levels in the synaptic cleft. Lithium may also have effects on other
neurotransmitter systems and neuromodulators.
Lithium's efficacy as an augmentation agent has been demonstrated in a series
of case studies that produced response rates of 30 to 65 percent. In some cases,
responses were noted within 48 hours, but delays of three to six weeks have also
been reported.
|
Patients who are most likely to benefit from the
substitution of an antidepressant medication are those who haven't
responded at all to the one they are now taking. |
The potential adverse effects of lithium are well known. They include hand
tremor, weight gain, increased thirst and urine production, and mild cognitive
impairment. A starting dosage of 150 mg twice daily, with a trough serum level
obtained within one week, is a practical starting point for augmentation
therapy. The lithium dosage should be adjusted to result in a serum blood level
between 0.4 and 0.8 mEq per L (0.4 and 0.8 mmol per L). In clinical practice,
aiming for the lower limit is prudent, since there is probably equal
augmentative efficacy at serum blood levels of 0.4 and 0.8 mEq per L (0.4 and
0.8 mmol per L). Attempting to enhance response by increasing the dosage to
higher serum blood levels may only result in unwanted side effects.
Thyroid hormone. The thyroid hormone triiodothyronine (T3
[Cytomel]) appears to be a more effective augmentation agent than
tetraiodothyronine (T4 [Synthroid]) and is
effective in small dosages; for example, 25 to 50 µg per day.14
T3 may be used to augment response to
tricyclic antidepressants, monoamine oxidase inhibitors and SSRIs. Although
fewer controlled studies have focused on thyroid hormone than on lithium, T3
augmentation of tricyclic antidepressants has been shown to be effective in
approximately 50 to 60 percent of patients.
Monitoring thyroid function before T3
administration (for a baseline reading) as well as after administration is
important. Beyond the observation that T3
potentiates noradrenergic activity, its mechanism of action as an augmentation
agent is not clearly understood. Although T3
is a relatively safe augmentation agent with few adverse effects or potential
allergic reactions, it has the potential, if taken chronically, to interfere
with thyroid metabolism. Therefore, its use should generally be limited to two
or three weeks. Adverse effects associated with excess administration of T3
include irritability, sweating and the possibility of cardiac arrhythmias.
Pindolol. The 5-HT1A postsynaptic
antagonist pindolol accelerates the onset of action of antidepressants by
preventing negative feedback to the presynaptic 5-HT1A
receptor. Prevention of negative feedback results in higher levels of serotonin
in the synapse. On a clinical level, pindolol, at dosages of 2.5 to 7.5 mg per
day for a trial period of up to six weeks, might prove to be an effective
augmentor of SSRIs. Adverse effects of pindolol, which occurred in fewer than 10
percent of study participants, included nausea, diarrhea and mild heart rate
reduction.
Buspirone. In terms of clinical characteristics, buspirone's primary
activity is as an anxiolytic. Although buspirone may decrease the nonspecific
symptoms of depression, it has no specific or intrinsic antidepressant effects.
However, when used in conjunction with an antidepressant, it may have
augmentative antidepressant effects. A number of open studies of dosages of 15
to 30 mg of buspirone per day for up to three months suggested that an improved
antidepressant response occurred in up to two thirds of patients. Adverse
effects of buspirone, including lightheadedness and nausea, usually occur early
and are generally transient.
Buspirone acts as a full agonist at the presynaptic autoreceptor and as a
partial agonist at the postsynaptic autoreceptor. Administration of buspirone
decreases extracellular serotonin concentrations over the short term through
activation of 5-HT1A presynaptic autoreceptors.
Buspirone also activates postsynaptic 5-HT1A
receptors. Chronic buspirone administration desensitizes and downregulates 5-HT1A
presynaptic autoreceptors, but not postsynaptic 5-HT1A
receptors, thereby encouraging further serotonin release.
Caution is necessary when prescribing buspirone with
nefazodone (Serzone).
Dizziness, insomnia and headaches may occur more frequently with this
combination than with either drug alone. This finding is likely related to the
fact that there is pharmacokinetic interaction between nefazodone (which
inhibits the cytochrome P450 enzyme 3A3/4) and buspirone (which is metabolized
by this enzyme). In order to avoid this potential interaction while still
deriving benefits from buspirone's augmentative effects with nefazodone, a lower
initial dosage of buspirone (2.5 mg, twice daily) should be prescribed.
Roger J. Cadieux, M.D.,
is associate professor of psychiatry and director of the geriatric assessment
program in the Department of Psychiatry at Pennsylvania State University College
of Medicine, Hershey.
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