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'Spatial heterogeneity of environmental risk in randomized prevention trials: consequences and modeling'

Authors :
Abdoulaye Guindo
Issaka Sagara
Boukary Ouedraogo
Kankoe Sallah
Mahamadoun Hamady Assadou
Sara Healy
Patrick Duffy
Ogobara K. Doumbo
Alassane Dicko
Roch Giorgi
Jean Gaudart
Source :
BMC Medical Research Methodology, Vol 19, Iss 1, Pp 1-16 (2019)
Publication Year :
2019
Publisher :
BMC, 2019.

Abstract

Abstract Background In the context of environmentally influenced communicable diseases, proximity to environmental sources results in spatial heterogeneity of risk, which is sometimes difficult to measure in the field. Most prevention trials use randomization to achieve comparability between groups, thus failing to account for heterogeneity. This study aimed to determine under what conditions spatial heterogeneity biases the results of randomized prevention trials, and to compare different approaches to modeling this heterogeneity. Methods Using the example of a malaria prevention trial, simulations were performed to quantify the impact of spatial heterogeneity and to compare different models. Simulated scenarios combined variation in baseline risk, a continuous protective factor (age), a non-related factor (sex), and a binary protective factor (preventive treatment). Simulated spatial heterogeneity scenarios combined variation in breeding site density and effect, location, and population density. The performances of the following five statistical models were assessed: a non-spatial Cox Proportional Hazard (Cox-PH) model and four models accounting for spatial heterogeneity—i.e., a Data-Generating Model, a Generalized Additive Model (GAM), and two Stochastic Partial Differential Equation (SPDE) models, one modeling survival time and the other the number of events. Using a Bayesian approach, we estimated the SPDE models with an Integrated Nested Laplace Approximation algorithm. For each factor (age, sex, treatment), model performances were assessed by quantifying parameter estimation biases, mean square errors, confidence interval coverage rates (CRs), and significance rates. The four models were applied to data from a malaria transmission blocking vaccine candidate. Results The level of baseline risk did not affect our estimates. However, with a high breeding site density and a strong breeding site effect, the Cox-PH and GAM models underestimated the age and treatment effects (but not the sex effect) with a low CR. When population density was low, the Cox-SPDE model slightly overestimated the effect of related factors (age, treatment). The two SPDE models corrected the impact of spatial heterogeneity, thus providing the best estimates. Conclusion Our results show that when spatial heterogeneity is important but not measured, randomization alone cannot achieve comparability between groups. In such cases, prevention trials should model spatial heterogeneity with an adapted method. Trial registration The dataset used for the application example was extracted from Vaccine Trial #NCT02334462 (ClinicalTrials.gov registry).

Details

Language :
English
ISSN :
14712288
Volume :
19
Issue :
1
Database :
Directory of Open Access Journals
Journal :
BMC Medical Research Methodology
Publication Type :
Academic Journal
Accession number :
edsdoj.51de8900a594b3e853de4484c0d4eb6
Document Type :
article
Full Text :
https://doi.org/10.1186/s12874-019-0759-z