Triiodothyronine Addition to Paroxetine in the Treatment of Major Depressive Disorder

Abstract

There is evidence that thyroid hormone T₃ increases serotonergic neurotransmission. Therefore, T₃ addition to antidepressants may improve treatment response in major depression. In nonrefractory depression, T₃ addition to tricyclic antidepressants indeed accelerates treatment response. Current therapeutic practice favors selective serotonin reuptake inhibitors. This is the first study to investigate the efficacy of T₃ addition to paroxetine in major depression. One hundred thirteen patients with major depressive disorder were randomly assigned to 8 wk of double-blind outpatient treatment with low-dose T₃ (25 μg), high-dose T₃ (25 μg twice daily), or placebo in addition to paroxetine 30 mg daily. A total of 106 patients started treatment and were included in the outcome analysis. Response rate after 8 wk (reduction of Hamilton Rating Scale for Depression score ≥ 50%) was 46% in all three treatment arms (P = 0.99). T₃ addition did not accelerate clinical response to paroxetine, nor was an effect of T₃ found when only women were analyzed. Patients on T₃ addition reported more adverse events than patients on placebo comedication. In conclusion, these results do not support a role for T₃ addition to selective serotonin reuptake inhibitors in the treatment of nonrefractory major depressive disorder. On the contrary, more adverse reactions occurred in T₃-treated patients.