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Inicio Revista de Psiquiatría y Salud Mental (English Edition) Tianeptine, antidepressant with positive benefit/risk
Journal Information
Vol. 9. Issue 4.
Pages 234-235 (October - December 2016)
Vol. 9. Issue 4.
Pages 234-235 (October - December 2016)
Letter to the Editor
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Tianeptine, antidepressant with positive benefit/risk
Tianeptina, antidepresivo con perfil beneficio/riesgo positivo
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Pilar García-García
Scientific Manager/QPPV, Juste SAQF, Coslada, Madrid, Spain
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Dear Editor,

In reply to the letter published in the Rev Psiquiatr Salud Ment (Barc.). 2016;9:176–177 by Calabozo et al.,1 under the title “Tianeptine: why has it not been classified as a narcotic in Spain?”, here in Juste SAQF we would like to express certain considerations. Firstly, Juste SAQF is a pharmaceutical company which commenced the commercialisation of medicines in the Spanish market in the year 1922, and since its origins it has always been characterised by strict compliance with the parameters that guarantee patient safety and well-being. Health is the chief objective of Juste, and therefore, according to the pharmacovigilance regulations in force, it monitors medicines and continuously and permanently evaluates their safety profile.

Tianeptina (Zinosal®) is a generic medicine which was authorised in Spain on 13/08/2014, and it is currently commercialised by our company. Tianeptine has been commercialised in France since 1988, and it is authorised in 15 European countries and in 66 countries around the world. The safety profile of Tianeptine is still monitored in the countries where it is authorised, and additionally, it is included in the EURD-list of the EMA for single evaluation of the Periodical Safety Report (PSUSA/00002943/201806; updated DLP: 04/03/2016).

This pharmacovigilance is fundamental given that, as with all medicines, adverse effects may arise which permit the evaluation of each drug in terms of its benefits and risks for each specific disease. In this respect, it is necessary to underline that the last revision undertaken by the French authorities on 5 December 2012, on Tianeptine, concluded that its benefit/risk ratio is still positive.2 Based on this evaluation, in the section of adverse reactions of the technical data sheet of Zinosal®, it is said that it may be involved in “substance abuse and dependency”, although it states that this basically involves a specific type of patient: “above all in patients under 50 years old with a history of drug or alcohol abuse”, while this adverse reaction is classified under the heading of “Rare” (>1/10,000 to >1/1000).

Two years later, in 2014, the French National Medicine and Health Products Safety Agency re-evaluated the information from 2012 to 2013, concluding that the number cases of abuse involving Tianeptine had fallen, given that only 7 cases3 had been described (ANSM, 2014).

Moreover, it is important to emphasise that Tianeptine has a different pharmacodynamic profile from those of current antidepressants,4,5 and that it has been proven in comparative studies to be more effective than a placebo and not inferior to tricylcic antidepressants or SSRI, with a more favourable tolerability profile.5–11

As the French public health authority (HAS) points out, Tianeptine2 has a positive benefit/risk ratio. Given that not all patients respond to existing antidepressant treatments, and given the clearly different action of Tianeptine on possible mechanisms that lead to an antidepressant effect, approval of its use in Spain represents a broadening of the spectrum of antidepressant treatment that has duly been authorised by the AEMPS for commercialisation under the commercial name of Zinosal®. Juste guarantees the pharmacovigilance of this drug in the same way that it does for all those within its catalogue.

References
[1]
B. Calabozo, V. Molina, F. Uribe.
Tianeptina: ¿por qué en España no ha sido catalogada como estupefaciente?.
Rev Psiquiatr Salud Ment (Barc), 9 (2016), pp. 174-177
[2]
Haute Autorité de Santé (HAS). Comission de la transparence. Avis, 5 December 2012. Available at: http://www.has-sante.fr/portail/upload/docs/evamed/CT2029_STABLON_ReevalSMR_avis2_CT10411_CT12029.pdf [accessed 04.07.16].
[3]
ANSM.
Comité technique des Centres d’Evaluation et d’Information sur la Pharmacodépendance-CT022013043 Zolad.
(2014),
[4]
B.S. McEwen, S. Chattarji, D.M. Diamond, T.M. Jay, L.P. Reagan, P. Svenningsson, et al.
The neurobiological properties of tianeptine (Stablon): from monoamine hypothesis to glutamatergic modulation.
Mol Psychiatry, 15 (2010), pp. 237-249
[5]
I. Yoo, J.M. Woo, S.H. Lee, M. Fava, D. Mischoulon, G.I. Papakostas, et al.
Influence of anxiety symptoms on improvement of neurocognitive functions in patients with major depressive disorder: a 12-week, multicenter, randomized trial of tianeptine versus escitalopram, the CAMPION study.
J Affect Disord, 185 (2015), pp. 24-30
[6]
H. Lôo, H. Ganry, H. Dufour, J.D. Guelfi, R. Malka, J.P. Olié, et al.
Long-term use of tianeptine in 380 depressed patients.
Br J Psychiatry Suppl, 15 (1992), pp. 61-65
[7]
J.D. Guelfi.
Efficacy of tianeptine in comparative trials versus reference antidepressants. An overview.
Br J Psychiatry Suppl, (1992), pp. 72-75
[8]
J.A. Costa e Silva, S.I. Ruschel, D. Caetano, F.L. Rocha, J.R. da Silva Lippi, S. Arruda, et al.
Placebo-controlled study of tianeptine in major depressive episodes.
Neuropsychobiology, 35 (1997), pp. 24-29
[9]
M. Bonierbale, C. Lancon, J. Tignol.
The ELIXIR study: evaluation of sexual dysfunction in 4557 depressed patients in France.
Curr Med Res Opin, 19 (2003), pp. 114-124
[10]
S. Kasper, B.S. McEwen.
Neurobiological and clinical effects of the antidepressant tianeptine.
CNS Drugs, 22 (2008), pp. 15-26
[11]
H.J. Jeon, J.M. Woo, S.H. Lee, E.J. Kim, S. Chung, J.H. Ha, et al.
Improvement in subjective and objective neurocognitive functions in patients with major depressive disorder: a 12-week, multicenter, randomized trial of tianeptine versus escitalopram, the CAMPION study.
J Clin Psychopharmacol, 34 (2014), pp. 218-225

Please cite this article as: García-García P. Tianeptina, antidepresivo con perfil beneficio/riesgo positivo. Rev Psiquiatr Salud Ment (Barc.). 2016;9:234–235.

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