4.5 Article

A dynamic model for estimating adult female mortality from ovarian dissection data for the tsetse fly Glossina pallidipes Austen sampled in Zimbabwe

Journal

PLOS NEGLECTED TROPICAL DISEASES
Volume 11, Issue 8, Pages -

Publisher

PUBLIC LIBRARY SCIENCE
DOI: 10.1371/journal.pntd.0005813

Keywords

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Funding

  1. NIGMS/MI DAS program [1-U01GM08778, F31GM120985]
  2. UNICEF/UNDP/World Bank/WHO Special Programme for Research and Training in Tropical Diseases
  3. Canadian International Development Research Centre
  4. DFID Animal Health Programme [R7539, R7987]
  5. DFID/RCUK programme on Zoonoses and Emerging Livestock Systems [BB/L019035/1]
  6. International Clinics on Infectious Disease Dynamics and Data [ICI3D]
  7. University of Florida's Emerging Pathogens Institute
  8. SACEMA
  9. NIH's National Institute of General Medical Sciences [R25GM102149]
  10. BBSRC [BB/L019035/1] Funding Source: UKRI

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Human and animal trypanosomiasis, spread by tsetse flies (Glossina spp), is a major public health concern in much of sub-Saharan Africa. The basic reproduction number of vector-borne diseases, such as trypanosomiasis, is a function of vector mortality rate. Robust methods for estimating tsetse mortality are thus of interest for understanding population and disease dynamics and for optimal control. Existing methods for estimating mortality in adult tsetse, from ovarian dissection data, often use invalid assumptions of the existence of a stable age distribution, and age-invariant mortality and capture probability. We develop a dynamic model to estimate tsetse mortality from ovarian dissection data in populations where the age distribution is not necessarily stable. The models correspond to several hypotheses about how temperature affects mortality: no temperature dependence (model 1), identical temperature dependence for mature adults and immature stages, i.e., pupae and newly emerged adults (model 2), and differential temperature dependence for mature adults and immature stages (model 3). We fit our models to ovarian dissection data for G. pallidipes collected at Rekomitjie Research Station in the Zambezi Valley in Zimbabwe. We compare model fits to determine the most probable model, given the data, by calculating the Akaike Information Criterion (AIC) for each model. The model that allows for a differential dependence of temperature on mortality for immature stages and mature adults (model 3) performs significantly better than models 1 and 2. All models produce mortality estimates, for mature adults, of approximately 3% per day for mean daily temperatures below 25 degrees C, consistent with those of mark-recapture studies performed in other settings. For temperatures greater than 25 degrees C, mortality among immature classes of tsetse increases substantially, whereas mortality remains roughly constant for mature adults. As a sensitivity analysis, model 3 was simultaneously fit to both the ovarian dissection and trap data; while this fit also produces comparable mortality at temperatures below 25 degrees C, it is not possible to obtain good fits to both data sources simultaneously, highlighting the uncertain correspondence between trap catches and population levels and/or the need for further improvements to our model. The modelling approach employed here could be applied to any substantial time series of age distribution data.

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