Multicrossover Randomized Controlled Trial Designs in <scp>A</scp>lzheimer Disease

Arnold, Steven E.; Betensky, Rebecca A.

doi:10.1002/ana.25280

Cited by 11 publications

(12 citation statements)

References 54 publications

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“…In addition to possible carry‐over effects, withdrawal effects and placebo responses are enmeshed and, as a result, our estimates of variability may partly reflect the variability of withdrawal effects. To disentangle withdrawal and placebo responses in cross‐over designs is complex but not impossible, and could be considered in studies aiming to further unpack individual variability of response 24 . The open‐label method also assumes that the change in symptom severity with an active compound following a period of placebo treatment is a fair estimate of the treatment effect; whether this is fully justified is not known, although our group‐level findings suggest that this may be a reasonable assumption.…”

Section: Discussionmentioning

confidence: 99%

Reappraising the variability of effects of antipsychotic medication in schizophrenia: a meta‐analysis

et al. 2022

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It is common experience for practising psychiatrists that individuals with schizophrenia vary markedly in their symptomatic response to antipsychotic medication. What is not clear, however, is whether this variation reflects variability of medication‐specific effects (also called “treatment effect heterogeneity”), as opposed to variability of non‐specific effects such as natural symptom fluctuation or placebo response. Previous meta‐analyses found no evidence of treatment effect heterogeneity, suggesting that a “one size fits all” approach may be appropriate and that efforts at developing personalized treatment strategies for schizophrenia are unlikely to succeed. Recent advances indicate, however, that earlier approaches may have been unable to accurately quantify treatment effect heterogeneity due to their neglect of a key parameter: the correlation between placebo response and medication‐specific effects. In the present paper, we address this shortcoming by using individual patient data and study‐level data to estimate that correlation and quantitatively characterize antipsychotic treatment effect heterogeneity in schizophrenia. Individual patient data (on 384 individuals who were administered antipsychotic treatment and 88 who received placebo) were obtained from the Yale University Open Data Access (YODA) database. Study‐level data were obtained from a meta‐analysis of 66 clinical trials including 17,202 patients. Both individual patient and study‐level analyses yielded a negative correlation between placebo response and treatment effect for the total score on the Positive and Negative Syndrome Scale (PANSS) (ρ=–0.32, p=0.002 and ρ=–0.39, p<0.001, respectively). Using the most conservative of these estimates, a meta‐analysis of treatment effect heterogeneity provided evidence of a marked variability in antipsychotic‐specific effects between individuals with schizophrenia, with the top quartile of patients experiencing beneficial treatment effects of 17.7 points or more on the PANSS total score, while the bottom quartile presented a detrimental effect of treatment relative to placebo. This evidence of clinically meaningful treatment effect heterogeneity suggests that efforts to personalize antipsychotic treatment of schizophrenia have potential for success.

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Section: Discussionmentioning

confidence: 99%

Reappraising the variability of effects of antipsychotic medication in schizophrenia: a meta‐analysis

et al. 2022

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“…The results of our n-of-1 trials without personalized interventions within the trial could be used to inform participants about their future dietary options. The design of the n-of-1 trial may also facilitate a detailed assessment about the sensitivity and specificity of an intervention, given that participants serve as their own controls in repeated crossover interventions, and all the analyses are based on personal outcomes for each individual ( 46 ). Furthermore, personal outcomes derived from the n-of-1 trial can be included in future clinical practice, which may enhance the clinical relevance of the treatment's effects.…”

Section: Discussionmentioning

confidence: 99%

Individual Postprandial Glycemic Responses to Diet in n-of-1 Trials: Westlake N-of-1 Trials for Macronutrient Intake (WE-MACNUTR)

Tian

et al. 2021

The Journal of Nutrition

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Background The role of different types and quantities of macronutrients on human health has been controversial, and the individual response to dietary macronutrient intake needs more investigation. Objectives We aimed to use an ‘n-of-1’ study design to investigate the individual variability in postprandial glycemic response when eating diets with different macronutrient distributions among apparently healthy adults. Methods Thirty apparently healthy young Chinese adults (women, 68%) aged between 22 and 34 y, with BMI between 17.2 and 31.9 kg/m2, were provided with high-fat, low-carbohydrate (HF-LC, 60–70% fat, 15–25% carbohydrate, 15% protein, of total energy) and low-fat, high-carbohydrate (LF-HC, 10–20% fat, 65–75% carbohydrate, 15% protein) diets, for 6 d wearing continuous glucose monitoring systems, respectively, in a randomized sequence, interspersed by a 6-d wash-out period. Three cycles were conducted. The primary outcomes were the differences of maximum postprandial glucose (MPG), mean amplitude of glycemic excursions (MAGE), and AUC24 between intervention periods of LF-HC and HF-LC diets. A Bayesian model was used to predict responders with the posterior probability of any 1 of the 3 outcomes reaching a clinically meaningful difference. Results Twenty-eight participants were included in the analysis. Posterior probability of reaching a clinically meaningful difference of MPG (0.167 mmol/L), MAGE (0.072 mmol/L), and AUC24 (13.889 mmol/L·h) between LF-HC and HF-LC diets varied among participants, and those with posterior probability >80% were identified as high-carbohydrate responders (n = 9) or high-fat responders (n = 6). Analyses of the Bayesian-aggregated n-of-1 trials among all participants showed a relatively low posterior probability of reaching a clinically meaningful difference of the 3 outcomes between LF-HC and HF-LC diets. Conclusions N-of-1 trials are feasible to characterize personal response to dietary intervention in young Chinese adults.

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“…In addition to possible carryover effects, withdrawal effects and placebo responses are enmeshed, and as a result our estimates of variability may partly reflect the variability of withdrawal effects. To disentangle withdrawal and placebo responses in crossover designs is complex but not impossible, and could be considered in studies aiming to further unpack individual variability of response (26). The open label method also assumes that the change in symptom severity with an active compound following a period of placebo treatment is a fair estimate of the treatment effect; whether this is fully justified is not known, although the group level findings suggest this may be a reasonable assumption.…”

Section: Limitationsmentioning

confidence: 99%

Reappraising Treatment Effect Heterogeneity in Schizophrenia: A Meta-analysis

McCutcheon

Pillinger

Efthimiou

et al. 2021

Preprint

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ObjectiveDetermining whether individual patients differ in response to treatment (‘treatment effect heterogeneity’) is important as it is a prerequisite to developing personalised treatment approaches. Previous variability meta-analyses of response to antipsychotics in schizophrenia found no evidence for treatment effect heterogeneity. Conversely, individual patient data meta-analyses suggest treatment effect heterogeneity does exist. In the current paper we combine individual patient data with study level data to resolve this apparent contradiction and quantitively characterise antipsychotic treatment effect heterogeneity in schizophrenia.MethodIndividual patient data (IPD) was obtained from the Yale University Open Data Access (YODA) project. Clinical trials were identified in EMBASE, PsycInfo, and PubMed. Treatment effect heterogeneity was estimated from variability ratios derived from study-level data from 66 RCTs of antipsychotics in schizophrenia (N=17,202). This estimation required a correlation coefficient (ρ) between placebo response and treatment effects to be estimated. We estimated this from both study level estimates of the 66 trials, and individual patient data (N=560).ResultsBoth individual patient (ρ=-0.32, p=0.002) and study level (ρ=-0.38, p<0.001) analyses yielded a negative correlation between placebo response and treatment effect. Using these estimates we found evidence of clinically significant treatment effect heterogeneity for total symptoms (our most conservative estimate was SD = 13.5 Positive and Negative Syndrome Scale (PANSS) points). Mean treatment effects were 8.6 points which, given the estimated SD, suggests the top quartile of patients experienced beneficial treatment effects of at least 17.7 PANSS points, while the bottom quartile received no benefit as compared to placebo.ConclusionsWe found evidence of clinically meaningful treatment effect heterogeneity for antipsychotic treatment of schizophrenia. This suggests efforts to personalise treatment have potential for success, and demonstrates that variability meta-analyses of RCTs need to account for relationships between placebo response and treatment effects.

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Multicrossover Randomized Controlled Trial Designs in Alzheimer Disease

Cited by 11 publications

References 54 publications

Reappraising the variability of effects of antipsychotic medication in schizophrenia: a meta‐analysis

Reappraising the variability of effects of antipsychotic medication in schizophrenia: a meta‐analysis

Individual Postprandial Glycemic Responses to Diet in n-of-1 Trials: Westlake N-of-1 Trials for Macronutrient Intake (WE-MACNUTR)

Reappraising Treatment Effect Heterogeneity in Schizophrenia: A Meta-analysis

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