Calcium, cyclic AMP and protein kinase C--partners in mitogenesis

Evidence is steadily mounting that the proto-oncogenes, whose products organize and start the programs that drive normal eukaryotic cells through their chromosome replication/mitosis cycles, are transiently stimulated by sequential signals from a multi-purpose, receptor-operated mechanism (consistin...

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Veröffentlicht in:Cancer and metastasis reviews 1987-01, Vol.5 (3), p.205-250
Hauptverfasser: Whitfield, J F, Durkin, J P, Franks, D J, Kleine, L P, Raptis, L, Rixon, R H, Sikorska, M, Walker, P R
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Sprache:eng
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Zusammenfassung:Evidence is steadily mounting that the proto-oncogenes, whose products organize and start the programs that drive normal eukaryotic cells through their chromosome replication/mitosis cycles, are transiently stimulated by sequential signals from a multi-purpose, receptor-operated mechanism (consisting of internal surges of Ca2+ and bursts of protein kinase C activity resulting from phosphatidylinositol 4,5-bisphosphate breakdown and the opening of membrane Ca2+ channels induced by receptor-associated tyrosine-protein kinase activity) and bursts of cyclic AMP-dependent kinase activity. The bypassing or subversion of the receptor-operated Ca2+/phospholipid breakdown/protein kinase C signalling mechanism is probably the basis of the freeing of cell proliferation from external controls that characterizes all neoplastic transformations.
ISSN:0167-7659
1573-7233
DOI:10.1007/BF00046999