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Comparing the evidential strength for psychotropic drugs: a Bayesian meta-analysis

Approval and prescription of psychotropic drugs should be informed by the strength of evidence for efficacy. Using a Bayesian framework, we examined (1) whether psychotropic drugs are supported by substantial evidence (at the time of approval by the Food and Drug Administration), and (2) whether the...

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Autores principales: Pittelkow, Merle-Marie, de Vries, Ymkje Anna, Monden, Rei, Bastiaansen, Jojanneke A., van Ravenzwaaij, Don
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Cambridge University Press 2021
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8640368/
https://www.ncbi.nlm.nih.gov/pubmed/34620261
http://dx.doi.org/10.1017/S0033291721003950
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author Pittelkow, Merle-Marie
de Vries, Ymkje Anna
Monden, Rei
Bastiaansen, Jojanneke A.
van Ravenzwaaij, Don
author_facet Pittelkow, Merle-Marie
de Vries, Ymkje Anna
Monden, Rei
Bastiaansen, Jojanneke A.
van Ravenzwaaij, Don
author_sort Pittelkow, Merle-Marie
collection PubMed
description Approval and prescription of psychotropic drugs should be informed by the strength of evidence for efficacy. Using a Bayesian framework, we examined (1) whether psychotropic drugs are supported by substantial evidence (at the time of approval by the Food and Drug Administration), and (2) whether there are systematic differences across drug groups. Data from short-term, placebo-controlled phase II/III clinical trials for 15 antipsychotics, 16 antidepressants for depression, nine antidepressants for anxiety, and 20 drugs for attention deficit hyperactivity disorder (ADHD) were extracted from FDA reviews. Bayesian model-averaged meta-analysis was performed and strength of evidence was quantified (i.e. BF(BMA)). Strength of evidence and trialling varied between drugs. Median evidential strength was extreme for ADHD medication (BF(BMA) = 1820.4), moderate for antipsychotics (BF(BMA) = 365.4), and considerably lower and more frequently classified as weak or moderate for antidepressants for depression (BF(BMA) = 94.2) and anxiety (BF(BMA) = 49.8). Varying median effect sizes (ES(schizophrenia) = 0.45, ES(depression) = 0.30, ES(anxiety) = 0.37, ES(ADHD) = 0.72), sample sizes (N(schizophrenia) = 324, N(depression) = 218, N(anxiety) = 254, N(ADHD) = 189.5), and numbers of trials (k(schizophrenia) = 3, k(depression) = 5.5, k(anxiety) = 3, k(ADHD) = 2) might account for differences. Although most drugs were supported by strong evidence at the time of approval, some only had moderate or ambiguous evidence. These results show the need for more systematic quantification and classification of statistical evidence for psychotropic drugs. Evidential strength should be communicated transparently and clearly towards clinical decision makers.
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spelling pubmed-86403682021-12-13 Comparing the evidential strength for psychotropic drugs: a Bayesian meta-analysis Pittelkow, Merle-Marie de Vries, Ymkje Anna Monden, Rei Bastiaansen, Jojanneke A. van Ravenzwaaij, Don Psychol Med Review Article Approval and prescription of psychotropic drugs should be informed by the strength of evidence for efficacy. Using a Bayesian framework, we examined (1) whether psychotropic drugs are supported by substantial evidence (at the time of approval by the Food and Drug Administration), and (2) whether there are systematic differences across drug groups. Data from short-term, placebo-controlled phase II/III clinical trials for 15 antipsychotics, 16 antidepressants for depression, nine antidepressants for anxiety, and 20 drugs for attention deficit hyperactivity disorder (ADHD) were extracted from FDA reviews. Bayesian model-averaged meta-analysis was performed and strength of evidence was quantified (i.e. BF(BMA)). Strength of evidence and trialling varied between drugs. Median evidential strength was extreme for ADHD medication (BF(BMA) = 1820.4), moderate for antipsychotics (BF(BMA) = 365.4), and considerably lower and more frequently classified as weak or moderate for antidepressants for depression (BF(BMA) = 94.2) and anxiety (BF(BMA) = 49.8). Varying median effect sizes (ES(schizophrenia) = 0.45, ES(depression) = 0.30, ES(anxiety) = 0.37, ES(ADHD) = 0.72), sample sizes (N(schizophrenia) = 324, N(depression) = 218, N(anxiety) = 254, N(ADHD) = 189.5), and numbers of trials (k(schizophrenia) = 3, k(depression) = 5.5, k(anxiety) = 3, k(ADHD) = 2) might account for differences. Although most drugs were supported by strong evidence at the time of approval, some only had moderate or ambiguous evidence. These results show the need for more systematic quantification and classification of statistical evidence for psychotropic drugs. Evidential strength should be communicated transparently and clearly towards clinical decision makers. Cambridge University Press 2021-12 2021-10-08 /pmc/articles/PMC8640368/ /pubmed/34620261 http://dx.doi.org/10.1017/S0033291721003950 Text en © The Author(s) 2021 https://creativecommons.org/licenses/by/4.0/This is an Open Access article, distributed under the terms of the Creative Commons Attribution licence (http://creativecommons.org/licenses/by/4.0/), which permits unrestricted re-use, distribution and reproduction, provided the original article is properly cited.
spellingShingle Review Article
Pittelkow, Merle-Marie
de Vries, Ymkje Anna
Monden, Rei
Bastiaansen, Jojanneke A.
van Ravenzwaaij, Don
Comparing the evidential strength for psychotropic drugs: a Bayesian meta-analysis
title Comparing the evidential strength for psychotropic drugs: a Bayesian meta-analysis
title_full Comparing the evidential strength for psychotropic drugs: a Bayesian meta-analysis
title_fullStr Comparing the evidential strength for psychotropic drugs: a Bayesian meta-analysis
title_full_unstemmed Comparing the evidential strength for psychotropic drugs: a Bayesian meta-analysis
title_short Comparing the evidential strength for psychotropic drugs: a Bayesian meta-analysis
title_sort comparing the evidential strength for psychotropic drugs: a bayesian meta-analysis
topic Review Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8640368/
https://www.ncbi.nlm.nih.gov/pubmed/34620261
http://dx.doi.org/10.1017/S0033291721003950
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