Acute and Longer-Term Outcomes in Depressed Outpatients Requiring One or Several Treatment Steps: A STAR*D Report

Rush, A. John; Trivedi, Madhukar H.; Wisniewski, Stephen R.; Nierenberg, Andrew A.; Stewart, Jonathan W.; Warden, Diane; Niederehe, George; Thase, Michael E.; Lavori, Philip W.; Lebowitz, Barry D.; McGrath, Patrick J.; Rosenbaum, Jerrold F.; Sackeïm, Harold A.; Kupfer, David J.; Luther, James F.; Fava, Maurizio

doi:10.1176/foc.6.1.foc128

Cited by 519 publications

(698 citation statements)

References 32 publications

(76 reference statements)

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“…The primary objective was to compare the efficacy of augmentation with risperidone vs. placebo in patients with difficult-to-treat depression, defined as patients who failed to respond or only partially responded to antidepressant monotherapy. We focused on difficultto-treat depression as a useful concept that may have more generalizability than TRD and, according to a recent STAR*D report, may be part of a continuum that leads to TRD (Thase et al, 2007;Rush et al, 2006). We selected 5 weeks as a lead-in period as it met the higher range of duration (3-5 weeks) defining an adequate treatment trial (Keller, 1988;Sackheim, 2001).…”

Section: Introductionmentioning

confidence: 99%

A randomized, placebo-controlled trial of risperidone augmentation for patients with difficult-to-treat unipolar, non-psychotic major depression

Keitner

Garlow

Ryan

et al. 2009

Journal of Psychiatric Research

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Objective-Patients (30-50%) with non-psychotic major depression will not respond despite an adequate trial of antidepressant medication. This study evaluated risperidone as an augmenting agent for patients who failed or only partially responded to an adequate trial of an antidepressant medication.Method-Ninety-seven patients with unipolar non-psychotic major depression who were not responsive to antidepressant monotherapy were randomized to risperidone (0.5-3 mg/day) or placebo augmentation in a four-week, double-blind, placebo controlled treatment trial. The primary outcome measure was remission defined by a score of ≤10 on the Montgomery-Asberg Depression Rating Scale (MADRS). Secondary outcomes measures were the Hamilton Rating Scale for Depression, the Clinician Global Impression of Severity scale and the overall satisfaction item of the Quality of Life and Enjoyment Questionnaire.Results-Subjects in both treatment groups improved significantly over time. The odds of remitting were significantly better for patients in the risperidone vs. placebo arm (OR = 3.33, p = . 011). At the end of 4 weeks of treatment 52% of the risperidone augmentation group remitted (MADRS ≤ 10) compared to 24% of the placebo augmentation group (CMH(1) = 6.48, p = .011), but the two groups were converging. Patients in the risperidone group also reported significantly more improvement in quality-of-life than patients in the placebo group. There were no betweengroup differences in the number of adverse events reported, however, weight gain was significantly higher in the group receiving risperidone. Conclusion-Augmentation of an antidepressant with risperidone for patients with difficult-totreat depression leads to more rapid response and a higher remission rate and better quality-of-life.

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Section: Introductionmentioning

confidence: 99%

A randomized, placebo-controlled trial of risperidone augmentation for patients with difficult-to-treat unipolar, non-psychotic major depression

Keitner

Garlow

Ryan

et al. 2009

Journal of Psychiatric Research

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“…While 80% of patients will experience partial relief of depressive symptoms, complete remission occurs in only 50-60% of all cases despite treatment with multiple antidepressants (Nestler et al, 2002;Rush et al, 2006). Even in patients who respond to drug therapy, chronic treatmentFon the order of weeks or monthsFis required before antidepressants provide clinical benefit.…”

Section: Introductionmentioning

confidence: 99%

Genetic Regulation of Behavioral and Neuronal Responses to Fluoxetine

Miller

Schultz

Gulati

et al. 2007

Neuropsychopharmacol

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Despite widespread use of antidepressants, the factors underlying the behavioral response to antidepressants are unknown. It has been shown that antidepressant treatment promotes the proliferation and survival of neurons in the adult hippocampus via enhanced serotonergic signaling, but it is unclear whether hippocampal neurogenesis is responsible for the behavioral response to antidepressants. Furthermore, a large subpopulation of patients fails to respond to antidepressant treatment due to presumed underlying genetic factors. In the present study, we have used the phenotypic and genotypic variability of inbred mouse strains to show that there is a genetic component to both the behavioral and neuronal effects of chronic fluoxetine treatment, and that this antidepressant induces an increase in hippocampal cell proliferation only in the strains that also show a positive behavioral response to treatment. Furthermore, the behavioral and neuronal responses are associated with an upregulation of genes known to promote neuronal proliferation and survival. These results suggest that inherent genetic predisposition to increased serotonin-induced neurogenesis may be a determinant of antidepressant efficacy.

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“…While newer antidepressants generally have fewer acute adverse effects and reduced overdose potential, their overall efficacy is still unacceptably low. 8 Pharmaceutical companies have therefore decided they cannot justify the huge investment they have been making in CNS research given the low likelihood of success in launching a safe drug with enhanced efficacy compared to the many other drugs already on the market. However, it is interesting that similar rates of failure are seen in other therapeutic areas, which are still being fully supported by pharmaceutical industry research (Figure 1).…”

Section: T He Meeting Of the Serotonin Club In July 2012 Inmentioning

confidence: 99%

How Do We Re-Engage the Pharmaceutical Industry in Research on Serotonin and Psychiatric Disorders?

Green

Marsden

2013

ACS Chem. Neurosci.

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The Serotonin Club celebrated its silver jubilee in 2012 with a meeting in Montpellier, France. During the past 25 years, great advances have been made in our understanding of the pharmacology of serotonin receptors and the roles of this neurotransmitter in psychiatric disorders. Most of these advances have involved effective collaborations between academic and industrial scientists. In recent years, however, this picture has changed, as many of the major pharmaceutical companies have pulled out of in-house psychopharmacology research into the major psychiatric disorders, despite an increasing worldwide burden of these disorders and a clear need for improved treatment, particularly in terms of improved efficacy. This Viewpoint investigates the reasons for the decline in industrial involvement and makes proposals as to how future academic research on serotonin function in the brain might reawaken industry interest in serotonin-based research. Briefly, academic preclinical scientists need to alter their experimental approach to research into the psychiatric disorders. This will require a move from a single-target approach to understanding the complex neuronal pathways the cause diverse functional and behavioral outputs, using novel technological advances and the development of animal models with enhanced translational values. It is hoped that such an approach will reveal novel drug targets and thus re-engage the pharmaceutical industry in research that will result in improved human health and social well-being.

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Acute and Longer-Term Outcomes in Depressed Outpatients Requiring One or Several Treatment Steps: A STAR*D Report

Cited by 519 publications

References 32 publications

A randomized, placebo-controlled trial of risperidone augmentation for patients with difficult-to-treat unipolar, non-psychotic major depression

A randomized, placebo-controlled trial of risperidone augmentation for patients with difficult-to-treat unipolar, non-psychotic major depression

Genetic Regulation of Behavioral and Neuronal Responses to Fluoxetine

How Do We Re-Engage the Pharmaceutical Industry in Research on Serotonin and Psychiatric Disorders?

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