Changes in Clinical Trials Methodology Over Time: A Systematic Review of Six Decades of Research in Psychopharmacology

Brunoni, André R.; Tadini, L.; Fregni, Felipe

doi:10.1371/journal.pone.0009479

Cited by 34 publications

(20 citation statements)

References 123 publications

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“…Overall, trial duration ranged from 0.1 to 260 weeks (median [IQR] 12 [8][9][10][11][12][13][14][15][16][17][18][19][20][21][22][23][24][25][26] Only eight diabetes trials (6.6%) enrolled subjects with type 1 diabetes (numbers not shown in tables). Table 3 presents results for the distribution of trial characteristics by the study outcome.…”

Section: Trial Characteristics and Study Outcomementioning

confidence: 99%

“…These studies generally failed to quantify the number of placebo-only-controlled trials, distinguish the presence of an additional placebo control group in a multi-armed trial, or assess whether subjects in the placebo group were required to be given concomitant or background therapy. [24][25][26][27][28][29][30] To our knowledge, the extent to which placebo-only versus active interventions are provided to control group subjects in clinical trials has not been examined across multiple diseases. This study attempts to fill this gap by systematically assessing the distribution and characteristics of placebo-only versus active-controlled clinical trials supporting FDA approvals of new drugs and biologics for nine common life-threatening diseases.…”

Section: Introductionmentioning

confidence: 99%

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Placebo-only-controlled versus active-controlled trials of new drugs for nine common life-threatening diseases

Sorscher¹,

AbuDagga²,

Almashat³

et al. 2018

OAJCT

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Purpose:The Food and Drug Administration (FDA) permits investigators to withhold active interventions from human subjects randomly assigned to control groups in clinical trials. The scope of this practice in trials for life-threatening diseases is unknown. We assessed the frequency and characteristics of trials providing control group subjects with active interventions versus those providing only placebos to control group subjects in trials supporting FDA approvals of new drugs for nine life-threatening diseases. Materials and methods:We reviewed the FDA's database of approved drug products and identified all new approvals from 2006 to 2011 for drugs or biological products indicated for asthma, bipolar disorder, chronic obstructive pulmonary disease (COPD), diabetes mellitus, hypertension, osteoporosis, Parkinson's disease, partial seizures, and schizophrenia. Then, we identified all trials described in FDA medical review documents for these approvals and abstracted information on trial characteristics and the interventions provided to control group subjects. Results: Of 508 included trials, 201 (39.6%) were placebo-only-controlled, meaning subjects in at least one control group did not receive an active intervention, and 307 (60.4%) were active-controlled, meaning subjects in all control groups received an active intervention. The total recorded enrollments in control groups provided with placebos only and in control groups provided with active interventions were 19,361 and 93,093 subjects, respectively. The proportion of placebo-only-controlled trials varied across diseases (P<0.001), ranging from 75.5% for COPD to 0% for partial seizures and osteoporosis. Placebo-only controls were used in 76.9% of trials for severe COPD, 56.4% of trials for severe hypertension, 43.8% of trials for moderate or severe persistent asthma, and 6.7% of trials for severely uncontrolled diabetes. Logistic regression analysis showed that longer trials were associated with lower odds of being placebo-only-controlled compared with shorter trials. Conclusion: Providing only placebos to control groups in trials for life-threatening diseases is a common practice, potentially entailing varying degrees of risk to subjects. Further research is warranted to assess the impact of this practice, particularly in trials of long duration and those involving subjects with severe disease.

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Section: Trial Characteristics and Study Outcomementioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

Placebo-only-controlled versus active-controlled trials of new drugs for nine common life-threatening diseases

Sorscher¹,

AbuDagga²,

Almashat³

et al. 2018

OAJCT

View full text Add to dashboard Cite

show abstract

“…Therefore, this issue can threaten internal validity by increasing effect sizes on all groups, but not necessarily diminish the generalizability of a NIBS-pharmacotherapy trial. Although a design with a placebo arm is methodologically sound, there is an important ethical concern: on one hand, placebo use has been ubiquitous in psychiatric research since the first controlled trials 60 years ago [25]; on the other hand, there is the risk of harming the principle of equipoise, which states that there should be 'genuine uncertainty' on the preferred treatment [26]. In fact, a recent meta-ana lysis demonstrated that pharmacological interventions and placebo present similar suicidal risk in short-term studies [27]; ethical committees usually demand that patients with severe suicidal ideation must not be enrolled in placebo trials, and that patients should be actively asked about suicidal thoughts throughout the trial, and be dropped-out if the suicidal risk is high.…”

Section: Placebo Responsementioning

confidence: 99%

Combination of noninvasive brain stimulation with pharmacotherapy

Brunoni

Valim

Fregni

2011

Expert Review of Medical Devices

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Noninvasive brain stimulation (NIBS) techniques are being increasingly investigated as a therapeutic approach for neuropsychiatric disorders. One method is to combine NIBS with pharmacotherapy to enhance the clinical effects or avoid an increase in drug dosages to decrease the incidence of side effects. However, few studies to date have investigated the relative and combined efficacy of NIBS with pharmacotherapy. Based on a literature review of previous studies and meta-analyses for major depression, we identified four randomized, controlled trials that tested the combination of NIBS with a new drug and two trials that directly compared NIBS versus pharmacotherapy. There was no study designed to address the relative efficacy of each intervention against placebo and against combined therapy. We discuss the methods and rationale of NIBS-pharmacotherapy trials, addressing some methodological aspects, including factorial design, recruitment, blinding, blinding assessment, placebo effect and quantitative aspects, such as power analysis, statistics and interaction effects. Our review of the methodology underlying NIBS-drug trials provides insights for the further clinical research development of NIBS in major depression.

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“…In 1960s and 1970s there are reports of a method of non-invasive brain stimulation named "brain polarization", quite similar to modern transcranial direct current stimulation (tDCS), which could enhance mood and alertness in healthy volunteers 3 and treat depression 4,5 . Later on, this method was largely abandoned, possibly due to the advancement of psychopharmacology 6 and the social stigma of electroconvulsive therapy (ECT) that hindered the development of other forms of non-invasive brain stimulation.…”

Section: Introductionmentioning

confidence: 99%

Novel neurotherapeutics in psychiatry: use and rationale of transcranial direct current stimulation in major depressive disorder

Moffa¹,

Valiengo²,

Shiozawa³

et al. 2014

Rev. psiquiatr. clín.

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Background: Transcranial direct current stimulation (tDCS) is a novel non-pharmacological intervention being investigated for the treatment of major depressive disorder (MDD). Objective: To perform an updated review of tDCS for MDD. Method: Systematic review in Medline/PubMed and other databases of all clinical studies evaluating the clinical efficacy of tDCS in MDD, from the first date available to December/2013. Results: Out of 55 articles, 24 were included, being 6 open-label studies; 8 randomized, double-blind, sham-controlled trials; 2 follow-up studies; 2 meta-analyses and 6 case reports. We observed an improvement of 20-40% in depressive symptoms, being slightly better in open studies. Five randomized clinical trials displayed positive results. The meta--analyses presented mixed results; although none included the study of that represents almost 50% of the evaluated sample. Open-label studies and case reports also investigated tDCS in bipolar depression, post-stroke depression and employed different parameters of stimulation. Discussion: TDCS is a novel, promising treatment for MDD. Definite evidence from large, ongoing clinical trials will be available in the next years.

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Changes in Clinical Trials Methodology Over Time: A Systematic Review of Six Decades of Research in Psychopharmacology

Cited by 34 publications

References 123 publications

Placebo-only-controlled versus active-controlled trials of new drugs for nine common life-threatening diseases

Placebo-only-controlled versus active-controlled trials of new drugs for nine common life-threatening diseases

Combination of noninvasive brain stimulation with pharmacotherapy

Novel neurotherapeutics in psychiatry: use and rationale of transcranial direct current stimulation in major depressive disorder

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