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Vagus Nerve Stimulation (VNS) for Treatment-Resistant
Depression:
Efficacy, Side Effects, and Predictors of Outcome
Sackeim HA, Rush AJ, George MS, Marangell
LB, Husain MM, Nahas Z, Johnson CR, Seidman S, Giller C, Haines S, Simpson RK
Jr, Goodman RR.
Department of Biological Psychiatry, New York
State Psychiatric Institute, 1051 Riverside Drive, New York, NY 10032,
USA.
This open pilot study of
vagus nerve stimulation (VNS) in 60
patients with treatment-resistant major
depressive episodes (MDEs) aimed to: 1) define the response rate; 2)
determine the profile of side effects; and, most importantly; 3) establish
predictors of clinical outcome. Participants were outpatients with nonatypical,
nonpsychotic, major
depressive or bipolar
disorder who had not responded to at least two medication trials from
different antidepressant classes in the current MDE.
While on stable medication regimens, the
patients completed a baseline period followed by device implantation. A 2-week,
single blind, recovery period (no stimulation) was followed by 10 weeks of VNS.
Of 59 completers (one patient improved during the recovery period), the
response rate was 30.5% for the primary HRSD(28) measure, 34.0% for the
Montgomery-Asberg Depression Rating Scale (MADRAS), and 37.3% for the Clinical
Global Impression-Improvement Score (CGI-I of 1 or 2). The most common side
effect was voice alteration or hoarseness, 55.0% (33/60), which was generally
mild and related to output current intensity.
History of treatment resistance was predictive
of VNS outcome. Patients who had never received ECT (lifetime) were 3.9 times
more likely to respond. Of the 13 patients who had not responded to more than
seven adequate antidepressant trials in the current MDE, none responded,
compared to 39.1% of the remaining 46 patients (p=.0057). Thus, VNS appears
to be most effective in patients with low to moderate, but not extreme,
antidepressant resistance.
Evidence concerning VNS' long-term therapeutic
benefits and tolerability will be critical in determining its role in
treatment-resistant depression.
Source: Neuropsychopharmacology 2001
Nov;25(5):713-28
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