Gini R, Pajouheshnia R, Hall G, Platt R, Setoguchi S, Bazelier M, Kaplan S, Zhou X, Lanes S, Man K, Li L, Burcu M, Roberto G, Dodd C, Duran C, Wientzek-Fleischmann A, Soman K, Lai E, Marinier K, Bennett D, Gardarsdottir H. Data source heterogeneity in multi-data base Pharmacoepidemiologic studies: an ISPE-sponsored scoping review. Poster presented at the 2022 ICPE Conference; August 26, 2022. Copenhagen, Denmark. [abstract] Pharmacoepidemiol Drug Saf. 2022 Sep 23; 31(S2):216. doi: 10.1002/pds.5518


BACKGROUND: Interpreting the findings of multi-data base studiesrequires a clear understanding of the context and purpose of data col-lection for each participating data source. There is currently no guid-ance for how heterogeneity between data sources (HDS) should bereported and leveraged upon. The DIVERSEscoping review on thistopic is sponsored by ISPE.

OBJECTIVES: To report on the selection for a scoping review to identifyliterature describing recommendations, or tools to describe, report onor leverage HDS for pharmacoepidemiologic research.

METHODS: We identified relevant literature published up to end 2021.We first selected a set of core papers, based on the expertise of theco-authors. We then executed three steps: 1) a snowball search of thereference lists of the core papers, 2) a PubMed search and 3) a web-based search for gray literature. Documents were reviewed in a stan-dardized process by independent pairs of reviewers; first title andabstract (TIAB), then full text review (FTR) if TIAB was of interest. Weexcluded documents if they met any of the following criteria: 1)described only clinical trials and not observational (or routinely col-lected) data sources, 2) reported only statistical methods to handleheterogeneity in results (e.g. meta-analysis), 3) applied pharmacoepi-demiologic studies that were not focussed on methodology or provid-ing guidance, 4) papers otherwise out of scope (e.g. pre-clinicalstudies). We included documents if they reported at least one of thefollowing: 1) relevant descriptions of multiple data sources, 2) tools toreport on HDS, 3) strategies to use HDS to improve evidence, 4) guid-ance on reporting HDS. The initial core papers were automaticallyincluded in the scoping review.

RESULTS: We selected 23 core documents and retrieved 687 docu-ments (total=710). After TIAB, 186 documents (27.1% of 687) were ncluded for FTR. After FTR, 50 (26.9% of 186) were included in thescoping review by the independent pair of assessors. Including thecore papers, a total of 73 documents entered the scoping review,42 (57.5%) included relevant descriptions of multiple data sources,42 (57.5%) included tools to report on HDS, 52 (71.2%) included strat-egies to use HDS to improve evidence, and 32 (43.8%) included guid-ance on reporting on HDS.

CONCLUSIONS: Among the reviewed papers, a minority included guid-ance on reporting diversity,while a higher number included descriptions, tools, and strategies.This set of papers will undergo further content analysis, to extractcommon themes and identify knowledge gaps. This scoping reviewwill eventually inform the development of a guidance paper.

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