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Differential inhibition by two hetrazepine PAF antagonists of acute inflammation in the mouse
Author(s) -
Henriques Maria G.M.O.,
Weg Vivian B.,
Martins Marco A.,
Silva Patricia M.R.,
Fernandes Patricia D.,
Cordeiro Renato S.B.,
Vargaftig B.B.
Publication year - 1990
Publication title -
british journal of pharmacology
Language(s) - English
Resource type - Journals
SCImago Journal Rank - 2.432
H-Index - 211
eISSN - 1476-5381
pISSN - 0007-1188
DOI - 10.1111/j.1476-5381.1990.tb14671.x
Subject(s) - platelet activating factor , pleurisy , pharmacology , antagonist , inflammation , in vivo , pleural cavity , medicine , chemistry , receptor antagonist , receptor , immunology , pleural effusion , biology , anatomy , microbiology and biotechnology
1 The injection of 100 or 300 μg of carrageenin into the mouse paw or pleural cavity produced a delayed inflammatory reaction at 48 h while platelet activating factor (PAF)‐induced paw oedema and pleurisy were maximal 30 min after its injection. 2 The PAF antagonist, WEB 2086, failed to inhibit mouse paw oedema and pleurisy induced by PAF, but reduced the first phase of oedema (1–4 h) induced by carrageenin without interfering with the second one (48–72 h). In contrast, another structurally‐related PAF antagonist, WEB 2170, inhibited dose‐dependently both oedema and pleurisy induced by PAF and by carrageenin (48 h). 3 Repeated injections of PAF into the mouse paw or pleural cavity led to significant auto‐desensitization. The animals desensitized to PAF and injected with carrageenin also displayed a significantly reduced oedema. 4 Our results suggest that PAF may be involved in the inflammatory response to carrageenin in mice. Furthermore, because the different receptor antagonists displayed distinct effects against PAF itself, different sites for in vivo interaction of PAF are available and are species‐ and drug‐dependent.