Abstract
Pneumonia is one of the leading causes of death worldwide. The course of the disease is often highly dynamic with unforeseen critical deterioration within hours in a relevant proportion of patients. Besides antibiotic treatment, novel adjunctive therapies are under development. Their additive value needs to be explored in preclinical and clinical studies and corresponding therapy schedules require optimization prior to introduction into clinical practice. Biomathematical modeling of the underlying disease and therapy processes might be a useful aid to support these processes. We here propose a biomathematical model of murine immune response during infection with Streptococcus pneumoniae aiming at predicting the outcome of different treatment schedules. The model consists of a number of non-linear ordinary differential equations describing the dynamics and interactions of the pulmonal pneumococcal population and relevant cells of the innate immune response, namely alveolar- and inflammatory macrophages and neutrophils. The cytokines IL-6 and IL-10 and the chemokines CCL2, CXCL1 and CXCL5 are considered as major mediators of the immune response. We also model the invasion of peripheral blood monocytes, their differentiation into macrophages and bacterial penetration through the epithelial barrier causing blood stream infections. We impose therapy effects on this system by modelling antibiotic therapy and treatment with the novel C5a-inactivator NOX-D19. All equations are derived by translating known biological mechanisms into equations and assuming appropriate response kinetics. Unknown model parameters were determined by fitting the predictions of the model to time series data derived from mice experiments with close-meshed time series of state parameters. Parameter fittings resulted in a good agreement of model and data for the experimental scenarios. The model can be used to predict the performance of alternative schedules of combined antibiotic and NOX-D19 treatment. We conclude that we established a comprehensive biomathematical model of pneumococcal lung infection, immune response and barrier function in mice allowing simulations of new treatment schedules. We aim to validate the model on the basis of further experimental data. We also plan the inclusion of further novel therapy principles and the translation of the model to the human situation in the near future.
Highlights
Streptococcus pneumoniae infections are life-threatening especially in children or elderly patients [1]
We recently proposed a biomathematical model of Streptococcus pneumoniae infection in mice [5] considering major cellular players of the innate immune response
Understanding disease dynamics and underlying patho-mechanisms is of utmost importance to improve outcome of pneumonia therapy
Summary
Streptococcus pneumoniae infections are life-threatening especially in children or elderly patients [1]. The disease can rapidly deteriorate within hours requiring immediate intensive care. Such fulminant disease courses only affect a part of the patient population and it is so far difficult to predict which patients are at high risk. New adjuvant therapy options are under development. For example the recently developed drug NOX-D19 spiegelmer targets C5a, a component of the complement system responsible for several proinflammatory effects including tissue injury [2]. It was observed in [3] that NOX-D19 reduces lung permeability in mice. Its relative contribution in combination with antibiotic treatment is not explored
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