Most endocrine cells secrete hormones as a result of Ca(2+)-regulated exocytosis, i.e., fusion of the membranes of hormone-containing secretory granules with the cell membrane, which allows the hormone molecules to escape to the extracellular space. As in neurons, electrical activity and cell depolarization open voltage-sensitive Ca(2+) channels, and the resulting Ca(2+) influx elevate the intracellular Ca(2+) concentration, which in turn causes exocytosis. Whereas the main molecular components involved in exocytosis are increasingly well understood, quantitative understanding of the dynamical aspects of exocytosis is still lacking. Due to the nontrivial spatiotemporal Ca(2+) dynamics, which depends on the particular pattern of electrical activity as well as Ca(2+) channel kinetics, exocytosis is dependent on the spatial arrangement of Ca(2+) channels and secretory granules. For example, the creation of local Ca(2+) microdomains, where the Ca(2+) concentration reaches tens of µM, are believed to be important for triggering exocytosis. Spatiotemporal simulations of buffered Ca(2+) diffusion have provided important insight into the interplay between electrical activity, Ca(2+) channel kinetics, and the location of granules and Ca(2+) channels. By confronting simulations with statistical time-to-event (or survival) regression analysis of single granule exocytosis monitored with TIRF microscopy, a direct connection between location and rate of exocytosis can be obtained at the local, single-granule level. To get insight into whole-cell secretion, simplifications of the full spatiotemporal dynamics have shown to be highly helpful. Here, we provide an overview of recent approaches and results for quantitative analysis of Ca(2+) regulated exocytosis of hormone-containing granules.
Recent advances in mathematical modeling and statistical analysis of exocytosis in endocrine cells
PEDERSEN, MORTEN GRAM;TAGLIAVINI, ALESSIA;CORTESE, GIULIANA;RIZ, MICHELA;MONTEFUSCO, FRANCESCO
2017
Abstract
Most endocrine cells secrete hormones as a result of Ca(2+)-regulated exocytosis, i.e., fusion of the membranes of hormone-containing secretory granules with the cell membrane, which allows the hormone molecules to escape to the extracellular space. As in neurons, electrical activity and cell depolarization open voltage-sensitive Ca(2+) channels, and the resulting Ca(2+) influx elevate the intracellular Ca(2+) concentration, which in turn causes exocytosis. Whereas the main molecular components involved in exocytosis are increasingly well understood, quantitative understanding of the dynamical aspects of exocytosis is still lacking. Due to the nontrivial spatiotemporal Ca(2+) dynamics, which depends on the particular pattern of electrical activity as well as Ca(2+) channel kinetics, exocytosis is dependent on the spatial arrangement of Ca(2+) channels and secretory granules. For example, the creation of local Ca(2+) microdomains, where the Ca(2+) concentration reaches tens of µM, are believed to be important for triggering exocytosis. Spatiotemporal simulations of buffered Ca(2+) diffusion have provided important insight into the interplay between electrical activity, Ca(2+) channel kinetics, and the location of granules and Ca(2+) channels. By confronting simulations with statistical time-to-event (or survival) regression analysis of single granule exocytosis monitored with TIRF microscopy, a direct connection between location and rate of exocytosis can be obtained at the local, single-granule level. To get insight into whole-cell secretion, simplifications of the full spatiotemporal dynamics have shown to be highly helpful. Here, we provide an overview of recent approaches and results for quantitative analysis of Ca(2+) regulated exocytosis of hormone-containing granules.File | Dimensione | Formato | |
---|---|---|---|
MBS_accepted.pdf
accesso aperto
Tipologia:
Preprint (submitted version)
Licenza:
Accesso libero
Dimensione
2.25 MB
Formato
Adobe PDF
|
2.25 MB | Adobe PDF | Visualizza/Apri |
Pubblicazioni consigliate
I documenti in IRIS sono protetti da copyright e tutti i diritti sono riservati, salvo diversa indicazione.