Joint modelling of time-to-clinical malaria and parasite count in a cohort in an endemic area

Christopher C Stanley; Lawrence N Kazembe; Andrea G Buchwald; Mavuto Mukaka; Don P Mathanga; Michael G Hudgens; Miriam K Laufer; Tobias F Chirwa

doi:10.7243/2053-7662-7-1

Joint modelling of time-to-clinical malaria and parasite count in a cohort in an endemic area

J Med Stat Inform. 2019:7:1. doi: 10.7243/2053-7662-7-1.

Authors

Christopher C Stanley^{1

2}, Lawrence N Kazembe³, Andrea G Buchwald⁴, Mavuto Mukaka^{5

6}, Don P Mathanga², Michael G Hudgens⁷, Miriam K Laufer⁴, Tobias F Chirwa¹

Affiliations

¹ School of Public Health, Faculty of Health Sciences, University of the Witwatersrand, Johannesburg, South Africa.
² Malaria Alert Center, University of Malawi College of Medicine, Blantyre, Malawi.
³ Department of Statistics, University of Namibia, Windhoek, Namibia.
⁴ Center for Vaccine Development and Global Health, University of Maryland School of Medicine, Baltimore, USA.
⁵ Oxford Centre for Tropical Medicine and Global Health, Oxford, United Kingdom.
⁶ Mahidol-Oxford Tropical Medicine Research Unit, Bangkok, Thailand.
⁷ Department of Biostatistics, Center for AIDS Research (CFAR), University of North Carolina Chapel Hill, North Carolina, USA.

Abstract

Background: In malaria endemic areas such as sub-Saharan Africa, repeated exposure to malaria results in acquired immunity to clinical disease but not infection. In prospective studies, time-to-clinical malaria and longitudinal parasite count trajectory are often analysed separately which may result in inefficient estimates since these two processes can be associated. Including parasite count as a time-dependent covariate in a model of time-to-clinical malaria episode may also be inaccurate because while clinical malaria disease frequently leads to treatment which may instantly affect the level of parasite count, standard time-to-event models require that time-dependent covariates be external to the event process. We investigated whether jointly modelling time-to-clinical malaria disease and longitudinal parasite count improves precision in risk factor estimates and assessed the strength of association between the hazard of clinical malaria and parasite count.

Methods: Using a cohort data of participants enrolled with uncomplicated malaria in Malawi, a conventional Cox Proportional Hazards (PH) model of time-to-first clinical malaria episode with time-dependent parasite count was compared with three competing joint models. The joint models had different association structures linking a quasi-Poisson mixed-effects of parasite count and event-time Cox PH sub-models.

Results: There were 120 participants of whom 115 (95.8%) had >1 follow-up visit and 100 (87.5%) experienced the episode. Adults >15 years being reference, log hazard ratio for children <5 years was 0.74 (95% CI: 0.17, 1.26) in the joint model with best fit vs. 0.62 (95% CI: 0.04, 1.18) from the conventional Cox PH model. The log hazard ratio for the 5-15 years was 0.72 (95% CI: 0.22, 1.22) in the joint model vs.0.63 (95% CI: 0.11, 1.17) in the Cox PH model. The area under parasite count trajectory was strongly associated with the risk of clinical malaria, with a unit increase corresponding to-0.0012 (95% CI: -0.0021, -0.0004) decrease in log hazard ratio.

Conclusion: Jointly modelling longitudinal parasite count and time-to-clinical malaria disease improves precision in log hazard ratio estimates compared to conventional time-dependent Cox PH model. The improved precision of joint modelling may improve study efficiency and allow for design of clinical trials with relatively lower sample sizes with increased power.

Keywords: Cox proportional hazards model; Prospective studies; clinical malaria; joint modelling; longitudinal data; malaria parasite; time-to-event.

Abstract

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