Network meta-analysis of randomized clinical trials: Reporting the proper summaries

Author:

Zhang Jing1,Carlin Bradley P1,Neaton James D1,Soon Guoxing G2,Nie Lei2,Kane Robert3,Virnig Beth A3,Chu Haitao1

Affiliation:

1. Division of Biostatistics, University of Minnesota School of Public Health, Minneapolis, MN, USA

2. Division of Biometrics IV, Office of Biometrics/OTS/CDER/FDA, Silver Spring, MD, USA

3. Division of Health Policy and Management, University of Minnesota School of Public Health, Minneapolis, MN, USA

Abstract

Background In the absence of sufficient data directly comparing multiple treatments, indirect comparisons using network meta-analyses (NMAs) can provide useful information. Under current contrast-based (CB) methods for binary outcomes, the patient-centered measures including the treatment-specific event rates and risk differences (RDs) are not provided, which may create some unnecessary obstacles for patients to comprehensively trade-off efficacy and safety measures. Purpose We aim to develop NMA to accurately estimate the treatment-specific event rates. Methods A Bayesian hierarchical model is developed to illustrate how treatment-specific event rates, RDs, and risk ratios (RRs) can be estimated. We first compare our approach to alternative methods using two hypothetical NMAs assuming a fixed RR or RD, and then use two published NMAs to illustrate the improved reporting. Results In the hypothetical NMAs, our approach outperforms current CB NMA methods in terms of bias. In the two published NMAs, noticeable differences are observed in the magnitude of relative treatment effects and several pairwise statistical significance tests from previous report. Limitations First, to facilitate the estimation, each study is assumed to hypothetically compare all treatments, with unstudied arms being missing at random. It is plausible that investigators may have selected treatment arms on purpose based on the results of previous trials, which may lead to ‘nonignorable missingness’ and potentially bias our estimates. Second, we have not considered methods to identify and account for potential inconsistency between direct and indirect comparisons. Conclusions The proposed NMA method can accurately estimate treatment-specific event rates, RDs, and RRs and is recommended.

Publisher

SAGE Publications

Subject

Pharmacology,General Medicine

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