G protein activation: a receptor-independent mode of action for cationic amphiphilic neuropeptides and venom peptides

The neuropeptide substance P, the venom peptide mastoparan and the synthetic polyamine compound 48/80 activate rat peritoneal mast cells, leading to rapid histamine release by exocytosis. Although these effects are inhibited by pertussis toxin and involve a transient increase in IP3, no selective me...

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Veröffentlicht in:Trends in pharmacological sciences (Regular ed.) 1990-09, Vol.11 (9), p.358-362
Hauptverfasser: Mousli, Mouaiak, Bueb, Jean-Luc, Bronner, Christian, Rouot, Bruno, Landry, Yves
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Sprache:eng
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Zusammenfassung:The neuropeptide substance P, the venom peptide mastoparan and the synthetic polyamine compound 48/80 activate rat peritoneal mast cells, leading to rapid histamine release by exocytosis. Although these effects are inhibited by pertussis toxin and involve a transient increase in IP3, no selective membrane receptors have been identified. However, it has recently been shown that these compounds activate G proteins in vitro. Here Yves Landry and colleagues discuss the proposal that direct activation of G protein is the physiological mechanism of action of substance P on rat peritoneal mast cells, this mechanism being mimicked by mastoparan and 48/80, and possibly by other cationic amphiphilic peptides such as kinins. These compounds might be of help m defining the interaction between membrane receptors and G proteins.
ISSN:0165-6147
1873-3735
DOI:10.1016/0165-6147(90)90179-C