| Literature DB >> 28502808 |
Katrien Oude Rengerink1, Shona Kalkman2, Susan Collier3, Antonio Ciaglia4, Sally D Worsley5, Alison Lightbourne4, Laurent Eckert6, Rolf H H Groenwold2, Diederick E Grobbee7, Elaine A Irving5.
Abstract
This paper addresses challenges of identifying, enrolling, and retaining participants in a trial conducted within a routine care setting. All patients who are potential candidates for the treatments in routine clinical practice should be considered eligible for a pragmatic trial. To ensure generalizability, the recruited sample should have a similar distribution of the treatment effect modifiers as the target population. In practice, this can be best achieved by including-within the selected sites-all patients without further selection. If relevant heterogeneity between subgroups is expected, increasing the relative proportion of the subgroup of patients in the heterogeneous trial could be considered (oversampling) or a separate trial in this subgroup can be planned. Selection will nevertheless occur. Low enrollment and loss to follow-up can introduce selection and can jeopardize validity as well as generalizability. Pragmatic trials are conducted in clinical practice rather than in a dedicated research setting, which could reduce recruitment rates. However, if a trial poses a minimal burden to the physician and the patient and routine clinical practice is maximally adhered to, the participation rate may be high and loss to follow-up will not be a specific problem for pragmatic trials.Entities:
Keywords: Enrollment; Participant; Pragmatic trial; Real-world evidence; Recruitment; Representativeness
Mesh:
Year: 2017 PMID: 28502808 DOI: 10.1016/j.jclinepi.2016.12.021
Source DB: PubMed Journal: J Clin Epidemiol ISSN: 0895-4356 Impact factor: 6.437