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DOI: 10.1055/s-2005-873160
Low-dose Trazodone Effective in Insomnia
Publication History
Received: 15.4.2005
Revised: 27.5.2005
Accepted: 6.6.2005
Publication Date:
27 September 2005 (online)
Although the risk of benzodiazepine dependence may be overstated, alternatives in the pharmacological treatment of chronic insomnia are certainly welcome. One such candidate is trazodone (TRZ), a second-generation triazolopyridine antidepressant that possesses significant anxiolytic and sedative activity resulting from 5-HT2 and alpha-1 receptor blockade [5]. The drug has been shown to improve sleep efficiency, total sleep duration, deep sleep duration, and REM sleep duration and to reduce the duration of awakenings and stage 2 sleep in depressed insomniac patients [4]. It was also found to be useful in antidepressant-induced insomnia [3] and after detoxification in patients with alcoholism [2].
However, patients frequently complain of secondary effects, such as vegetative symptoms before sleep (tachycardia), very deep sleep (sometimes accompanied by incontinence), or prolonged hangover. As a result, several of them do not keep a positive image of this drug and wish to discontinue it.
A logical strategy was to use lower dosages than are commonly prescribed (50-100 mg).
Ten patients who had used trazodone at these dosages and appreciated its sleep-inducing and -maintaining properties but suffered from unwelcome secondary effects were invited to participate in an open trial. Using 5-mg capsules, they were asked to titrate their medication, in order to find the optimal balance between positive and negative effects. Two patients described their sleep as satisfying using as little as 5 mg of the substance; four, with 10 mg; three, with 15 mg; and one, with 20 mg).
According to these preliminary data, there is some reason to believe that trazodone is marketed at too high a dosage with regard to its sleep-acting properties, at least for a good fraction of the cases. Open-label and controlled studies should naturally confirm these findings. The potential overdosage, in turn, may provide a poor clinical impression of this otherwise quite valuable alternative to classical sleeping pills. This medication should be prescribed with a start-up strategy in mind, using very low dosages at first and remaining at that level in a certain number of cases.
Such a strategy is also in line with the new paradigms of individualized medicine, which suggests putting more stress on adjusting drug dosages as a function of a patient’s reaction, which is itself probably based a good deal on genetic variability [1].
References
- 1 Kirchheiner J, Bertilsson L, Bruus H, Wolff A, Roots I, Bauer M. Individualized medicine - implementation of pharmacogenetic diagnostics in antidepressant drug treatment of major depressive disorders. Pharmacopsychiatry. 2003; 36 (3) S235-S243
- 2 Le Bon O, Murphy J R, Staner L, Hoffmann G, Kormoss N, Kentos M, Dupont P h, Lion K, Pelc I, Verbanck P. A double-blind, placebo-controlled study of the efficacy of trazodone in alcohol post-withdrawal syndrome: polysomnographic and clinical evaluations. J Clin Psychopharmacol. 2003; 23 (4) 377-383
- 3 Nierenberg A A, Adler L A, Peselow E. et al . Trazodone for antidepressant-associated insomnia. Am J Psychiatry. 1994; 151 (7) 1069-1072
- 4 Saletu-Zyhlarz G M, Abu-Bakr M H, Anderer P. et al . Insomnia in depression: differences in objective and subjective sleep and awakening quality to normal controls and acute effects of trazodone. Prog Neuropsychopharmacol Biol Psychiatry. 2002; 26 (2) 249-260
- 5 Silvestrini B, Valeri P. Trazodone, a new avenue in the treatment of depression. Psychopathology. 1984; 17 (suppl 2) 3-14
Olivier Le Bon, MD, PhD
CHU Brugmann
Service de Psychiatrie
Pl. Van Gehuchten 4
1020 Bruxelles
02/477.29.17
Email: lebono@skynet.be