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To the Editor: A 2010 meta-analysis (1) concluded that reboxetine, a selective norepinephrine reuptake inhibitor approved for the treatment of depression in several countries worldwide, is “an ineffective and potentially harmful antidepressant.” Wide variation in the side effect profiles of therapeutic drugs makes the risk-to-benefit ratio for populations difficult to interpret. Greater understanding of the factors underlying such variation may facilitate the more effective selection of patients at lower risk of adverse events. For instance, both the therapeutic and adverse effects of reboxetine derive from enhanced norepinephrine transmission mediated by adrenergic receptors (adrenoceptors). The α2 group of adrenoceptors influences a range of human physiological functions, and the α2B subtype plays a specific role in the peripheral regulation of cardiovascular responses (2). We therefore hypothesized that a functional deletion polymorphism in the gene coding the α2B adrenoceptor (ADRA2B) (3) that has been linked to individual differences in norepinephrine signaling (4, 5) may mediate the adverse cardiovascular effects of norepinephrine reuptake inhibitors such as reboxetine.
In a study approved by the Brighton and Sussex Medical School Research Governance and Ethics Committee, 58 healthy male Caucasian volunteers 18 to 32 years old were genotyped for the ADRA2B deletion polymorphism. We recorded baseline cardiovascular parameters (pulse rate and systolic and diastolic blood pressure) and the severity of adverse effects (dry mouth, anxiety, sweating, palpitations, nausea, dizziness, irritability, and tiredness) using a visual analogue scale before administering either 4 mg of reboxetine (N=30) or placebo (N=28), using a double-blind procedure. Two hours later, in keeping with the tmax for reboxetine, we repeated cardiovascular and adverse effect measures (posttreatment). In addition to a main effect of reboxetine on pulse rate (F=7.6, df=1, 53, p=0.005) and total adverse effect score (F=11.4, df=1, 53, p=0.001), we observed a significant interaction between ADRA2B genotype and the severity of posttreatment adverse effects (F=5.0, df=1, 53, p=0.03), while correcting for baseline measurements. In participants lacking a copy of the ADRA2B deletion variant (N=24; 12 each in the reboxetine and placebo groups), reboxetine was associated with a significant increase in adverse effect scores from baseline (t=3.7, df=22, p=0.001) that was absent in participants with at least one copy of the deletion allele (N=34; 18 in the reboxetine group and 16 in the placebo group) (see Figure 1). In the reboxetine group, the number needed to treat (by genotyping) to prevent an increase of ≥50 in the adverse effect score was 2.6.
FIGURE 1. Influence of ADRA2B Genotype on Adverse Effect Severity Scores in Placebo (N=28; 16 in the Deletion Group and 12 in the No Deletion Group) and Reboxetine (N=30; 18 in the Deletion Group and 12 in the No Deletion Group) Groups
a Significant difference in adverse effect severity scores (t=3.7, df=22, p=0.001).
To our knowledge, this is the first report of a genetic moderator of severity of adverse effects following a single dose of reboxetine. It is also one of the first reports of a genetically determined pharmacodynamic marker of psychotropic drug adverse effects (6). Further studies to replicate and extend our findings (including chronic dosing and patient populations) and to clarify the underlying mechanisms will be necessary for clinical application. However, the utility of such data is likely to extend beyond reboxetine to other selective norepinephrine reuptake inhibitors currently on the market (atomoxetine) and in late-stage development (edivoxetine).

References

1.
Eyding D, Lelgemann M, Grouven U, Härter M, Kromp M, Kaiser T, Kerekes MF, Gerken M, Wieseler B: Reboxetine for acute treatment of major depression: systematic review and meta-analysis of published and unpublished placebo and selective serotonin reuptake inhibitor controlled trials. BMJ 2010; 341:c4737
2.
Philipp M, Brede M, Hein L: Physiological significance of α(2)-adrenergic receptor subtype diversity: one receptor is not enough. Am J Physiol Regul Integr Comp Physiol 2002; 283:R287–R295
3.
Small KM, Brown KM, Forbes SL, Liggett SB: Polymorphic deletion of three intracellular acidic residues of the alpha 2B-adrenergic receptor decreases G protein-coupled receptor kinase-mediated phosphorylation and desensitization. J Biol Chem 2001; 276:4917–4922
4.
de Quervain DJF, Kolassa IT, Ertl V, Onyut PL, Neuner F, Elbert T, Papassotiropoulos A: A deletion variant of the α2b-adrenoceptor is related to emotional memory in Europeans and Africans. Nat Neurosci 2007; 10:1137–1139
5.
Naudts KH, Azevedo RT, David AS, van Heeringen K, Gibbs AA: Epistasis between 5-HTTLPR and ADRA2B polymorphisms influences attentional bias for emotional information in healthy volunteers. Int J Neuropsychopharmacol 2012; 15:1027–1036
6.
Kirchheiner J, Nickchen K, Bauer M, Wong ML, Licinio J, Roots I, Brockmöller J: Pharmacogenetics of antidepressants and antipsychotics: the contribution of allelic variations to the phenotype of drug response. Mol Psychiatry 2004; 9:442–473

Information & Authors

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Published In

Go to American Journal of Psychiatry
Go to American Journal of Psychiatry
American Journal of Psychiatry
Pages: 446b - 447
PubMed: 23545803

History

Accepted: January 2013
Published online: 1 April 2013
Published in print: April 2013

Authors

Details

Ayana A. Gibbs, M.B.Ch.B., Ph.D.
From the Division of Clinical Medicine, Brighton and Sussex Medical School, Falmer, Brighton, U.K.; the Institute of Psychiatry, King’s College London, King’s Health Partners, London; the School of Psychology, University of Sussex, Falmer, Brighton; and the Department of Psychiatry and Medical Psychology, Ghent University, Belgium.
Sirpreet K. Somal, B.Sc.
From the Division of Clinical Medicine, Brighton and Sussex Medical School, Falmer, Brighton, U.K.; the Institute of Psychiatry, King’s College London, King’s Health Partners, London; the School of Psychology, University of Sussex, Falmer, Brighton; and the Department of Psychiatry and Medical Psychology, Ghent University, Belgium.
Ki Fung D. Chan
From the Division of Clinical Medicine, Brighton and Sussex Medical School, Falmer, Brighton, U.K.; the Institute of Psychiatry, King’s College London, King’s Health Partners, London; the School of Psychology, University of Sussex, Falmer, Brighton; and the Department of Psychiatry and Medical Psychology, Ghent University, Belgium.
Carla E. Bautista, B.Sc., M.Sc
From the Division of Clinical Medicine, Brighton and Sussex Medical School, Falmer, Brighton, U.K.; the Institute of Psychiatry, King’s College London, King’s Health Partners, London; the School of Psychology, University of Sussex, Falmer, Brighton; and the Department of Psychiatry and Medical Psychology, Ghent University, Belgium.
Florence D. Mowlem
From the Division of Clinical Medicine, Brighton and Sussex Medical School, Falmer, Brighton, U.K.; the Institute of Psychiatry, King’s College London, King’s Health Partners, London; the School of Psychology, University of Sussex, Falmer, Brighton; and the Department of Psychiatry and Medical Psychology, Ghent University, Belgium.
Kris H. Naudts, M.D., Ph.D.
From the Division of Clinical Medicine, Brighton and Sussex Medical School, Falmer, Brighton, U.K.; the Institute of Psychiatry, King’s College London, King’s Health Partners, London; the School of Psychology, University of Sussex, Falmer, Brighton; and the Department of Psychiatry and Medical Psychology, Ghent University, Belgium.
Kees van Heeringen, M.D., Ph.D.
From the Division of Clinical Medicine, Brighton and Sussex Medical School, Falmer, Brighton, U.K.; the Institute of Psychiatry, King’s College London, King’s Health Partners, London; the School of Psychology, University of Sussex, Falmer, Brighton; and the Department of Psychiatry and Medical Psychology, Ghent University, Belgium.
Theodora Duka, M.D., Ph.D.
From the Division of Clinical Medicine, Brighton and Sussex Medical School, Falmer, Brighton, U.K.; the Institute of Psychiatry, King’s College London, King’s Health Partners, London; the School of Psychology, University of Sussex, Falmer, Brighton; and the Department of Psychiatry and Medical Psychology, Ghent University, Belgium.

Competing Interests

The authors report no financial relationships with commercial interests.

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