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Crosstalk between cellular morphology and calcium oscillation patterns Insights from a stochastic computer model
Authors:Michael Kraus, Bj  rn Wolf,Bernhard Wolf
Affiliation:Michael Kraus, Björn Wolf,Bernhard Wolf,
Abstract:Agonist-induced oscillations in the concentration of intracellular free calcium ([Ca2+]1) display a wide variety of temporal and spatial patterns. In non-excitable cells, typical oscillatory patterns are somewhat cell-type specific and range from frequency-encoded, repetitive Ca2+ spikes to oscillations that are more sinusoidal in shape. Although the response of a cell population, even to the same stimulus, is often extremely heterogeneous, the response of the same cell to successive exposures can be remarkably similar. We propose that such ‘Ca 2+ fingerprints’ can be a consequence of cell-specific morphological properties. The hypothesis is tested by means of a stochastic computer simulation of a two-dimensional model for oscillatory Ca 2+ waves which encompasses the basic elements of the two-pool oscillator introduced by Goldbeter et al. (Goldbeter A., Dupont G., Berridge M.J. Minimal model for signal-induced Ca2+-oscillations and for their frequency encoding through protein phosphorylation. Proc Natl Acad Sci USA 1990; 87: 1461–1465). In the framework of our extended spatiotemporal model, single cells can display various oscillation patterns which depend on the agonist dose, Ca2+ diffusibility, and several morphological parameters. These are, for example, size and shape of the cell and the cell nucleus, the amount and distribution of Ca2+ stores, and the subcellular location of the inositol(1,4,5)-trisphosphate-generating apparatus.
Keywords:Abbreviations: CICR, Ca2+-induced Ca 2+ release   CICRP, CICR pool   IICR, Insp3induced Ca2+ release   InsP3, inositol(1,4,5)-trisphosphate   ISCS, InsP3 sensitive Ca2+ store   PDE, partial differential equation
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