Abstract
Randomised clinical trials (RCTs) are the gold standard for providing unbiased evidence of intervention effects. Here, we provide an overview of the history of RCTs and discuss the major challenges and limitations of current critical care RCTs, including overly optimistic effect sizes; unnuanced conclusions based on dichotomization of results; limited focus on patient-centred outcomes other than mortality; lack of flexibility and ability to adapt, increasing the risk of inconclusive results and limiting knowledge gains before trial completion; and inefficiency due to lack of re-use of trial infrastructure. We discuss recent developments in critical care RCTs and novel methods that may provide solutions to some of these challenges, including a research programme approach (consecutive, complementary studies of multiple types rather than individual, independent studies), and novel design and analysis methods. These include standardization of trial protocols; alternative outcome choices and use of core outcome sets; increased acceptance of uncertainty, probabilistic interpretations and use of Bayesian statistics; novel approaches to assessing heterogeneity of treatment effects; adaptation and platform trials; and increased integration between clinical trials and clinical practice. We outline the advantages and discuss the potential methodological and practical disadvantages with these approaches. With this review, we aim to inform clinicians and researchers about conventional and novel RCTs, including the rationale for choosing one or the other methodological approach based on a thorough discussion of pros and cons. Importantly, the most central feature remains the randomisation, which provides unparalleled restriction of confounding compared to non-randomised designs by reducing confounding to chance.
| Originalsprog | Engelsk |
|---|---|
| Tidsskrift | Intensive Care Medicine |
| Vol/bind | 48 |
| Udgave nummer | 2 |
| Sider (fra-til) | 164-178 |
| ISSN | 0342-4642 |
| DOI | |
| Status | Udgivet - 2022 |
Bibliografisk note
Funding Information:The Department of Intensive Care at Copenhagen University Hospital—Rigshospitalet (AG, AP, MHM) has received grants from the Novo Nordisk Foundation, Pfizer, Fresenius Kabi and Sygeforsikringen “danmark” outside the submitted work. The University Medical Center Utrecht (LD) has received grants from the European Commission (Rapid European COVID-19 Emergency research Response (RECOVER) Grant number H2020 – 101003589; European Clinical Research Alliance on Infectious Diseases (ECRAID) Grant number H2020-965313) and the Dutch funder ZonMW (ANAkinra voor de behandeling van CORonavirus infectious disease 2019 op de Intensive Care (ANACOR-IC)Grant Number 10150062010003) for REMAP-CAP. FGZ has received grants for investigator initiated clinical trials from Ionis Pharmaceuticals (USA) and Bactiguard (Sweden), all unrelated to this work. The Critical Care Division, The George Institute for Global Health (NEH) has received grants from Baxter, CSL, and Fresenius Kabi outside the submitted work. EA declares having received fees for lectures from Alexion, Sanofi, Baxter, and Pfizer. His institution has received research grants from Fisher&Payckle, MSD and Baxter.
Funding Information:
This work received no specific funding. WA holds a McMaster University Department of Medicine Mid-Career Research Award. NEH is supported by a National Health and Medical Research Emerging Leader Grant (APP1196320). This research was conducted during the tenure of a Health Research Council of New Zealand Clinical Practitioner Research Fellowship held by PJY. The Medical Research Institute of New Zealand receives independent research organisation funding from the Health Research Council of New Zealand.
Publisher Copyright:
© 2021, Springer-Verlag GmbH Germany, part of Springer Nature.