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Defining the relationship between Plasmodium falciparum parasite rate and clinical disease: statistical models for disease burden estimation

Abstract:
Background: Clinical malaria has proven an elusive burden to enumerate. Many cases go undetected by routine disease recording systems. Epidemiologists have, therefore, frequently defaulted to actively measuring malaria in population cohorts through time. Measuring the clinical incidence of malaria longitudinally is labour-intensive and impossible to undertake universally. There is a need, therefore, to define a relationship between clinical incidence and the easier and more commonly measured index of infection prevalence: the "parasite rate". This relationship can help provide an informed basis to define malaria burdens in areas where health statistics are inadequate. Methods: Formal literature searches were conducted for Plasmodium falciparum malaria incidence surveys undertaken prospectively through active case detection at least every 14 days. The data were abstracted, standardized and geo-referenced. Incidence surveys were time-space matched with modelled estimates of infection prevalence derived from a larger database of parasite prevalence surveys and modelling procedures developed for a global malaria endemicity map. Several potential relationships between clinical incidence and infection prevalence were then specified in a non-parametric Gaussian process model with minimal, biologically informed, prior constraints. Bayesian inference was then used to choose between the candidate models. Results: The suggested relationships with credible intervals are shown for the Africa and a combined American and Central and South East Asia regions. In both regions clinical incidence increased slowly and smoothly as a function of infection prevalence. In Africa, when infection prevalence exceeded 40%, clinical incidence reached a plateau of 500 cases per thousand of the population per annum. In the combined America and Central and South East Asia regions, this plateau was reached at 250 cases per thousand of the population per annum. A temporal volatility model was also incorporated to facilitate a closer description of the variance in the observed data. Conclusion: It was possible to model a relationship between clinical incidence and P. falciparum infection prevalence but the best-fit models were very noisy reflecting the large variance within the observed opportunistic data sample. This continuous quantification allows for estimates of the clinical burden of P. falciparum of known confidence from wherever an estimate of P. falciparum prevalence is available.
Publication status:
Published
Peer review status:
Peer reviewed

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Institution:
University of Oxford
Division:
MPLS
Department:
Zoology
Research group:
Spatial Ecology and Epidemiology Group
Role:
Author
More by this author
Institution:
Centre for Geographic Medicine, KEMRI - University of Oxford - Wellcome Trust Collaborative Programme, Kenyatta National Hospital Grounds, Nairobi, Kenya
Research group:
"Wellcome Trust", "Kenyan Medical Research Institute"
Department:
Malaria Public Health and Epidemiology Group
Role:
Author
More by this author
Institution:
University of Oxford
Division:
MPLS
Department:
Zoology
Research group:
Spatial Ecology and Epidemiology Group
Role:
Author
More by this author
Institution:
University of Oxford
Division:
MPLS
Department:
Zoology
Research group:
Spatial Ecology and Epidemiology Group
Role:
Author
More by this author
Institution:
National Institute of Malaria Research (Indian Council of Medical Research), Field station, Orissa, India
Role:
Author


More from this funder
Funding agency for:
Patil, A
Gething, P
Guerra, C


Publisher:
BioMed Central
Journal:
Malaria Journal More from this journal
Volume:
8
Article number:
186
Publication date:
2009-08-01
Edition:
Publisher's version
DOI:
ISSN:
1475-2875


Language:
English
Subjects:
UUID:
uuid:ea7c31a8-920d-4f18-9606-aff73136aa14
Local pid:
ora:3661
Deposit date:
2010-04-23
ARK identifier:

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