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,< Peter Ahnert>,< Sandra Wienhold>,< Holger Mueller-Redetzky>,< ¿Ü> Àú | ¾ÆÁø

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2020-07-13
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Pneumonia is considered to be one of the leading causes of death worldwide. The
outcome depends on both, proper antibiotic treatment and the effectivity of the
immune response of the host. However, due to the complexity of the immunologic
cascade initiated during infection, the latter cannot be predicted easily. We
construct a biomathematical model of the murine immune response during infection
with pneumococcus aiming at predicting the outcome of antibiotic treatment. The
model consists of a number of non-linear ordinary differential equations describing
dynamics of pneumococcal population, the inflammatory cytokine IL-6, neutrophils
and macrophages fighting the infection and destruction of alveolar tissue due to
pneumococcus. Equations were derived by translating known biological mechanisms
and assuming certain response kinetics. Antibiotic therapy is modelled by a
transient depletion of bacteria. Unknown model parameters were determined by
fitting the predictions of the model to data sets derived from mice experiments of
pneumococcal lung infection with and without antibiotic treatment. Time series of
pneumococcal population, debris, neutrophils, activated epithelial cells,
macrophages, monocytes and IL-6 serum concentrations were available for this
purpose. The antibiotics Ampicillin and Moxifloxacin were considered. Parameter
fittings resulted in a good agreement of model and data for all experimental
scenarios. Identifiability of parameters is also estimated. The model can be used to
predict the performance of alternative schedules of antibiotic treatment. We
conclude that we established a biomathematical model of pneumococcal lung
infection in mice allowing predictions regarding the outcome of different schedules
of antibiotic treatment. We aim at translating the model to the human situation in
the near future.

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DC ¸ðÅÍÀÇ ½Ã¹Ä·¹ÀÌ¼Ç 24
ÇÔ¼ö ºí·ÏÀÇ »ç¿ë 29
Â÷ºÐ¹æÁ¤½Ä(difference equation)ÀÇ ¸ðµ¨¸µ 34
Subsystem(ºÎ½Ã½ºÅÛ)ÀÇ ±¸¼º 37

Á¦ 2Æí : ¿¬±¸³í¹®
A Biomathematical Model of Pneumococcal Lung Infection and
Antibiotic Treatment in Mice

1. Introduction 42
2. Methods 42
3. Modelling pharmacokinetics of antibiotics 46
4. Numerical Methods for Simulation 46
5. Results 49
6. Parameter sensitivity 51
7. Discussion 55
8. References 61