A mathematical model of T lymphocyte calcium dynamics derived from single transmembrane protein properties
Fate decision processes of T lymphocytes are crucial for health and disease. Whether a T lymphocyte is activated, divides, gets anergic or initiates apoptosis depends on extracellular triggers and intracellular signalling. Free cytosolic calcium dynamics plays an important role in this context. The...
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Frontiers Media S.A.
2013-09-01
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| Series: | Frontiers in Immunology |
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| Online Access: | http://journal.frontiersin.org/Journal/10.3389/fimmu.2013.00277/full |
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doaj-0722cd51f2ef4a0cbcab10c32949421f2020-11-24T21:40:20ZengFrontiers Media S.A.Frontiers in Immunology1664-32242013-09-01410.3389/fimmu.2013.0027761094A mathematical model of T lymphocyte calcium dynamics derived from single transmembrane protein propertiesChristine Dorothee Schmeitz0Esteban Abelardo Hernandez-Vargas1Ralf eFliegert2Andreas H Guse3Michael eMeyer-Hermann4Michael eMeyer-Hermann5Helmholtz Centre for Infection ResearchHelmholtz Centre for Infection ResearchUniversity Medical Center Hamburg-EppendorfUniversity Medical Center Hamburg-EppendorfHelmholtz Centre for Infection ResearchTechnische Universität BraunschweigFate decision processes of T lymphocytes are crucial for health and disease. Whether a T lymphocyte is activated, divides, gets anergic or initiates apoptosis depends on extracellular triggers and intracellular signalling. Free cytosolic calcium dynamics plays an important role in this context. The relative contributions of store-derived calcium entry and calcium entry from extracellular space to T lymphocyte activation are still a matter of debate. Here we develop a quantitative mathematical model of T lymphocyte calcium dynamics in order to establish a tool which allows to disentangle cause-effect relationships between ion fluxes and observed calcium time courses. The model is based on single transmembrane protein characteristics which have been determined in independent experiments. This reduces the number of unknown parameters in the model to a minimum and ensures the predictive power of the model. Simulation results are subsequently used for an analysis of whole cell calcium dynamics measured under various experimental conditions. The model accounts for a variety of these conditions, which supports the suitability of the modelling approach. The simulation results suggest a model in which calcium dynamics dominantly relies on the opening of channels in calcium stores while calcium entry through calcium-release activated channels (CRAC) is more associated with the maintenance of the T lymphocyte calcium levels and prevents the cell from calcium depletion. Our findings indicate that CRAC guarantees a long-term stable calcium level which is required for cell survival and sustained calcium enhancement.http://journal.frontiersin.org/Journal/10.3389/fimmu.2013.00277/fullEndoplasmic ReticulumT lymphocytesmathematical modelcalcium dynamicsCRAC |
| collection |
DOAJ |
| language |
English |
| format |
Article |
| sources |
DOAJ |
| author |
Christine Dorothee Schmeitz Esteban Abelardo Hernandez-Vargas Ralf eFliegert Andreas H Guse Michael eMeyer-Hermann Michael eMeyer-Hermann |
| spellingShingle |
Christine Dorothee Schmeitz Esteban Abelardo Hernandez-Vargas Ralf eFliegert Andreas H Guse Michael eMeyer-Hermann Michael eMeyer-Hermann A mathematical model of T lymphocyte calcium dynamics derived from single transmembrane protein properties Frontiers in Immunology Endoplasmic Reticulum T lymphocytes mathematical model calcium dynamics CRAC |
| author_facet |
Christine Dorothee Schmeitz Esteban Abelardo Hernandez-Vargas Ralf eFliegert Andreas H Guse Michael eMeyer-Hermann Michael eMeyer-Hermann |
| author_sort |
Christine Dorothee Schmeitz |
| title |
A mathematical model of T lymphocyte calcium dynamics derived from single transmembrane protein properties |
| title_short |
A mathematical model of T lymphocyte calcium dynamics derived from single transmembrane protein properties |
| title_full |
A mathematical model of T lymphocyte calcium dynamics derived from single transmembrane protein properties |
| title_fullStr |
A mathematical model of T lymphocyte calcium dynamics derived from single transmembrane protein properties |
| title_full_unstemmed |
A mathematical model of T lymphocyte calcium dynamics derived from single transmembrane protein properties |
| title_sort |
mathematical model of t lymphocyte calcium dynamics derived from single transmembrane protein properties |
| publisher |
Frontiers Media S.A. |
| series |
Frontiers in Immunology |
| issn |
1664-3224 |
| publishDate |
2013-09-01 |
| description |
Fate decision processes of T lymphocytes are crucial for health and disease. Whether a T lymphocyte is activated, divides, gets anergic or initiates apoptosis depends on extracellular triggers and intracellular signalling. Free cytosolic calcium dynamics plays an important role in this context. The relative contributions of store-derived calcium entry and calcium entry from extracellular space to T lymphocyte activation are still a matter of debate. Here we develop a quantitative mathematical model of T lymphocyte calcium dynamics in order to establish a tool which allows to disentangle cause-effect relationships between ion fluxes and observed calcium time courses. The model is based on single transmembrane protein characteristics which have been determined in independent experiments. This reduces the number of unknown parameters in the model to a minimum and ensures the predictive power of the model. Simulation results are subsequently used for an analysis of whole cell calcium dynamics measured under various experimental conditions. The model accounts for a variety of these conditions, which supports the suitability of the modelling approach. The simulation results suggest a model in which calcium dynamics dominantly relies on the opening of channels in calcium stores while calcium entry through calcium-release activated channels (CRAC) is more associated with the maintenance of the T lymphocyte calcium levels and prevents the cell from calcium depletion. Our findings indicate that CRAC guarantees a long-term stable calcium level which is required for cell survival and sustained calcium enhancement. |
| topic |
Endoplasmic Reticulum T lymphocytes mathematical model calcium dynamics CRAC |
| url |
http://journal.frontiersin.org/Journal/10.3389/fimmu.2013.00277/full |
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