A placebo-controlled comparison of the antidepressant efficacy and effects
on sexual functioning of sustained-release bupropion and sertraline
by
Haddjeri N, Blier P, de Montigny C
Croft H, Settle E Jr, Houser T, Batey SR, Donahue RM, Ascher JA
Charleston Area Medical Center, West Virginia, USA.
Clin Ther 1999 Apr; 21(4):643-58
ABSTRACT
Sexual dysfunction, a frequently reported side effect of many
antidepressants, may result in patient dissatisfaction and noncompliance with
treatment regimens. This paper describes the results of the first
placebo-controlled comparison of the efficacy, safety, and effects on sexual
functioning of sustained-release bupropion (bupropion SR) and the selective
serotonin reuptake inhibitor sertraline. This randomized, double-masked,
double-dummy, parallel-group, multicenter trial enrolled 360 patients with
moderate-to-severe recurrent major depression. Patients were treated with
bupropion SR 150 to 400 mg/d, sertraline 50 to 200 mg/d, or placebo for up to 8
weeks. Patients' depression and sexual functioning were assessed at weekly or
biweekly clinic visits; safety was assessed by regular monitoring of adverse
events, vital signs, and body weight. Treatment groups were similar at baseline
in terms of age, sex, and race, and most patients had a diagnosis of moderate
uncomplicated depression. Patients treated with bupropion SR or sertraline
showed similar improvements on all efficacy measures; both active treatments
were superior to placebo in improving scores on all rating scales for depression
at various time points. Significantly more patients treated with sertraline
experienced orgasmic dysfunction throughout the study than did patients treated
with bupropion SR or placebo (P < 0.001). Headache was the most frequently
reported adverse event in all 3 treatment groups and occurred with similar
frequency in each group (30% to 40%). Nausea (31%), diarrhea (26%), insomnia
(18%), and somnolence (17%) occurred in significantly more patients in the
sertraline group than in the bupropion SR group (18%, 7%, 13%, and 3%,
respectively) and the placebo group (10%, 11%, 4%, and 6%, respectively). Dry
mouth occurred more frequently with bupropion SR (19%) than with sertraline
(14%) or placebo (12%), although the differences were not significant. Changes
in vital signs were similar in all groups. Similar (small, but not statistically
significant) decreases in mean body weight were seen in both the bupropion SR
(-1.06 kg) and sertraline (-0.79 kg) groups, whereas the placebo group
experienced a minor increase (0.21 kg). Although bupropion SR and sertraline
were similarly well tolerated and effective in the treatment of depression,
sertraline treatment was more often associated with sexual dysfunction and
certain other adverse events compared with bupropion SR and placebo. Therefore,
bupropion SR may be an appropriate choice as an antidepressant for the treatment
of sexually active patients.
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