Spatiotemporal characteristics of calcium dynamics in astrocytes
Although Ca i 2 + waves in networks of astrocytes in vivo are well documented, propagation in vivo is much more complex than in culture, and there is no consensus concerning the dominant roles of intercellular and extracellular messengers [inositol 1,4,5–trisphosphate ( IP 3 ) and adenosine-5′-triph...
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Veröffentlicht in: | Chaos (Woodbury, N.Y.) N.Y.), 2009-09, Vol.19 (3), p.037116-037116-21 |
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Format: | Artikel |
Sprache: | eng |
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Zusammenfassung: | Although
Ca
i
2
+
waves in networks of astrocytes in vivo are well documented, propagation in vivo is much more complex than in culture, and there is no consensus concerning the dominant roles of intercellular and extracellular messengers [inositol 1,4,5–trisphosphate (
IP
3
) and adenosine-5′-triphosphate (ATP)] that mediate
Ca
i
2
+
waves. Moreover, to date only simplified models that take very little account of the geometrical struture of the networks have been studied. Our aim in this paper is to develop a mathematical model based on realistic cellular morphology and network connectivity, and a computational framework for simulating the model, in order to address these issues. In the model,
Ca
i
2
+
wave propagation through a network of astrocytes is driven by
IP
3
diffusion between cells and ATP transport in the extracellular space. Numerical simulations of the model show that different kinetic and geometric assumptions give rise to differences in
Ca
i
2
+
wave propagation patterns, as characterized by the velocity, propagation distance, time delay in propagation from one cell to another, and the evolution of
Ca
2
+
response patterns. The temporal
Ca
i
2
+
response patterns in cells are different from one cell to another, and the
Ca
i
2
+
response patterns evolve from one type to another as a
Ca
i
2
+
wave propagates. In addition, the spatial patterns of
Ca
i
2
+
wave propagation depend on whether
IP
3
, ATP, or both are mediating messengers. Finally, two different geometries that reflect the in vivo and in vitro configuration of astrocytic networks also yield distinct intracellular and extracellular kinetic patterns. The simulation results as well as the linear stability analysis of the model lead to the conclusion that
Ca
i
2
+
waves in astrocyte networks are probably mediated by both intercellular
IP
3
transport and nonregenerative (only the glutamate-stimulated cell releases ATP) or partially regenerative extracellular ATP signaling. |
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ISSN: | 1054-1500 1089-7682 |
DOI: | 10.1063/1.3206698 |