The role of clinical variables, neuropsychological performance and SLC6A4 and COMT gene polymorphisms on the prediction of early response to fluoxetine in major depressive disorder.

Esteve Gudayol-Ferré Ixchel Herrera-Guzmán Beatriz Camarena Carlos Cortés-Penagos Jorge E Herrera-Abarca Patricia Martínez-Medina David Cruz Sandra Hernández Alma Genis Mariana Y Carrillo-Guerrero Rubén Avilés Reyes Joan Guàrdia-Olmos

J Affect Disord

Clínica de Enfermedades Crónicas y Procedimientos Especiales CECYPE, Morelia, Mich., Mexico.

Published: December 2010

Major depressive disorder (MDD) treatment often involves antidepressants like fluoxetine, but only 50-70% of patients show an initial positive response; the study aims to identify predictive factors for treatment response.
Among clinical variables, only the presence of comorbid anxiety disorders indicated a poor response, while a combination of attention and planning performance helped predict a good response to fluoxetine.
The study highlights that while certain psychological factors can effectively classify treatment responders, the genetic variables examined did not predict treatment outcomes, and limitations such as potential placebo effects were noted.

Introduction: Major depressive disorder (MDD) is treated with antidepressants, but only between 50% and 70% of the patients respond to the initial treatment. Several authors suggested different factors that could predict antidepressant response, including clinical, psychophysiological, neuropsychological, neuroimaging, and genetic variables. However, these different predictors present poor prognostic sensitivity and specificity by themselves. The aim of our work is to study the possible role of clinical variables, neuropsychological performance, and the 5HTTLPR, rs25531, and val108/58Met COMT polymorphisms in the prediction of the response to fluoxetine after 4weeks of treatment in a sample of patient with MDD.

Methods: 64 patients with MDD were genotyped according to the above-mentioned polymorphisms, and were clinically and neuropsychologically assessed before a 4-week fluoxetine treatment. Fluoxetine response was assessed by using the Hamilton Depression Rating Scale. We carried out a binary logistic regression model for the potential predictive variables.

Results: Out of the clinical variables studied, only the number of anxiety disorders comorbid with MDD have predicted a poor response to the treatment. A combination of a good performance in variables of attention and low performance in planning could predict a good response to fluoxetine in patients with MDD. None of the genetic variables studied had predictive value in our model.

Limitations: The possible placebo effect has not been controlled. Our study is focused on response prediction but not in remission prediction.

Conclusions: Our work suggests that the combination of the number of comorbid anxiety disorders, an attentional variable, and two planning variables makes it possible to correctly classify 82% of the depressed patients who responded to the treatment with fluoxetine, and 74% of the patients who did not respond to that treatment.

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http://dx.doi.org/10.1016/j.jad.2010.06.002	DOI Listing

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