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Abstract

Introduction:

Bayesian adaptive designs for clinical trials have gained popularity in the recent years due to the flexibility and efficiency that they offer. We consider the scenario where the outcome of interest comprises events with relatively low risk of occurrence and different case definitions resulting in varying control group risk assumptions. This is a scenario that occurs frequently for infectious diseases in global health research.

Methods:

We propose a Bayesian adaptive design that incorporates different case definitions of the outcome of interest that vary in stringency. A set of stopping rules are proposed where superiority and futility may be concluded with respect to different outcome definitions and therefore maintain a realistic probability of stopping in trials with low event rates. Through a simulation study, a variety of stopping rules and design configurations are compared.

Results:

The simulation results are provided in an interactive web application that allows the user to explore and compare the design operating characteristics for a variety of assumptions and design parameters with respect to different outcome definitions. The results for select simulation scenarios are provided in the article.

Discussion:

Bayesian adaptive designs offer the potential for maximizing the information learned from the data collected through clinical trials. The proposed design enables monitoring and utilizing multiple composite outcomes based on rare events to optimize the trial design operating characteristics.

Keywords

Composite outcomes stopping rules futility superiority simulations

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References

Cheng

Shen

Bayesian adaptive designs for clinical trials. Biometrika 2005; 92: 633–646.

Berry

Carlin

Lee

, et al. Bayesian adaptive methods for clinical trials. Boca Raton, FL: CRC Press, 2010.

Harrington

Parmigiani

I-SPY 2 — a glimpse of the future of phase 2 drug development. N Engl J Med 2016; 375(1): 7–9.

Warner

Weir

Hansen

, et al. Low-dose dexamethasone as a treatment for women with heavy menstrual bleeding: protocol for response-adaptive randomised placebo-controlled dose-finding parallel group trial (DexFEM). BMJ Open 2015; 5(1): e006837.

Satlin

Wang

Logovinsky

, et al. Design of a Bayesian adaptive phase 2 proof-of-concept trial for BAN2401, a putative disease-modifying monoclonal antibody for the treatment of Alzheimer’s disease. Alzheimers Dement 2016; 2(1): 1–12.

Food and Drug Administration (FDA). Multiple endpoints in clinical trials: guidance for industry, 2017, https://www.fda.gov/files/drugs/published/Multiple-Endpoints-in-Clinical-Trials-Guidance-for-Industry.pdf

McCoy

CE.

Understanding the use of composite endpoints in clinical trials. West J Emerg Med 2018; 19(4): 631–634.

Mehta

Gao

Bhatt

, et al. Optimizing trial design: sequential, adaptive, and enrichment strategies. Circulation 2009; 119(4): 597–605.

Shane

Sanchez

Stoll

BJ.

Neonatal sepsis. Lancet 2017; 390: 1770–1780.

10.

Wynn

JL.

Defining neonatal sepsis. Curr Opin Pediatr 2016; 28(2): 135–140.

11.

Singer

Deutschman

Seymour

, et al. The third international consensus definitions for sepsis and septic shock (Sepsis-3). JAMA 2016; 315: 801–810.

12.

Vergnano

Buttery

Cailes

, et al. Neonatal infections: case definition and guidelines for data collection, analysis, and presentation of immunisation safety data. Vaccine 2016; 34: 6038–6046.

13.

Vergnano

Seale

Fitchett

EJA

, et al. Serious bacterial infections in neonates: improving reporting and case definitions. Int Health 2017; 9(3): 148–155.

Supplementary Material

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