Differential routes of Ca2+ influx in Swiss 3T3 fibroblasts in response to receptor stimulation

Differential routes of Ca2+ influx in Swiss 3T3 fibroblasts in response to receptor stimulation

Ca2+ influx into cells in response to stimulation of various receptors was studied with Swiss 3T3 fibroblasts. The mechanisms involved were found to be so diverse that they were classified into four groups, Type I to IV. Type-I influx occurred, via pertussis toxin-susceptible G-proteins, immediately...

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Veröffentlicht in:Biochemical journal 1998-01, Vol.329 ( Pt 1) (1), p.107-114
Hauptverfasser: Miyakawa, T, Kojima, M, Ui, M
Format: Artikel
Sprache:eng
Schlagworte:
3T3 Cells
Alprostadil - pharmacology
Angiotensin II - pharmacology
Animals
Arachidonic Acid - metabolism
Bombesin - pharmacology
Bradykinin - pharmacology
Calcium - metabolism
Calcium Channel Blockers - pharmacology
Diltiazem - pharmacology
Endothelins - pharmacology
Enzyme Activation - physiology
GTP-Binding Proteins - metabolism
Inositol Phosphates - metabolism
Mice
Nifedipine - pharmacology
Pertussis Toxin
Phospholipases A - metabolism
Phospholipases A2
Platelet-Derived Growth Factor - pharmacology
Protein Kinase C - metabolism
Receptors, Cell Surface - classification
Receptors, Cell Surface - metabolism
Tetradecanoylphorbol Acetate - pharmacology
Thapsigargin - pharmacology
Thrombin - pharmacology
Vasopressins - pharmacology
Virulence Factors, Bordetella - pharmacology
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Zusammenfassung:Ca2+ influx into cells in response to stimulation of various receptors was studied with Swiss 3T3 fibroblasts. The mechanisms involved were found to be so diverse that they were classified into four groups, Type I to IV. Type-I influx occurred, via pertussis toxin-susceptible G-proteins, immediately after internal Ca2+ mobilization by bradykinin, thrombin, endothelin, vasopressin or angiotensin II. Type-II influx induced by bombesin differed from Type I in its insusceptibility to pertussis toxin treatment. Ca2+ influx induced by prostaglandin E1, referred to as Type-III influx, was unique in that phospholipase C was apparently not activated without extracellular Ca2+, strongly suggesting that the Ca2+ influx preceded and was responsible for InsP3 generation and internal Ca2+ mobilization. More Ca2+ entered the cells more slowly via the Type-IV route opened by platelet-derived and other growth factors. These types of Ca2+ influx could be differentiated by their different susceptibilities to protein kinase C maximally activated by 1 h of exposure of cells to PMA, which inhibited phospholipase Cbeta coupled to receptors involved in Type-I and -II influx but did not inhibit growth-factor-receptor-coupled phospholipase Cgamma. Type-I and -II Ca2+ influxes, together with store-operated influx induced by thapsigargin, were not directly inhibited by exposure of cells to PMA, but Type-III and -IV influxes were completely inhibited. In addition, stimulation of receptors involved in Type-I and -IV Ca2+ influx, but not Type-II and -III influx, led to phospholipase A2 activation in the presence of extracellular Ca2+. Inhibition of Type-I and -IV Ca2+ influxes by their respective inhibitors, diltiazem and nifedipine, resulted in abolition of phospholipase A2 activation induced by the respective receptor agonists, in agreement with the notion that Ca2+ influx via these routes is responsible for receptor-mediated phospholipase A2 activation.
ISSN:0264-6021
1470-8728
DOI:10.1042/bj3290107