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Effect of structural analogues of PAF‐acether on platelet desensitization
Author(s) -
Keraly C. Lalau,
Coëffier E.,
Tencé M.,
Borrel M. C.,
Benveniste J.
Publication year - 1983
Publication title -
british journal of haematology
Language(s) - English
Resource type - Journals
SCImago Journal Rank - 1.907
H-Index - 186
eISSN - 1365-2141
pISSN - 0007-1048
DOI - 10.1111/j.1365-2141.1983.tb02053.x
Subject(s) - chemistry , platelet activating factor , stereochemistry , steric effects , desensitization (medicine) , agonist , ether , platelet , enantiomer , arachidonic acid , alkoxy group , pharmacology , medicinal chemistry , biochemistry , alkyl , receptor , organic chemistry , immunology , enzyme , biology
S ummary . The 1‐O‐alkyl‐2‐O‐acetyl‐sn‐glyceryl‐3‐phosphorylcholine (PAF‐acether) aggregates rabbit platelets and desensitizes them to a second challenge with the same agonist but not to arachidonic acid. The desensitizing activities of 14 analogues of PAF‐acether were explored with particular attention to the dose‐response dependency of the desensitization process. PAF‐acether was 500‐fold more active than its 1‐O‐acyl analogues. The 2‐lyso PAF‐acether was inactive and the PAF‐acether enantiomer 2000 times less effective than the natural isomer, thus confirming the importance of the presence and steric position of the 2‐acetate group. The desensitizing activities of the 2‐propionyl and the 2‐butyryl analogues were close to that of PAF‐acether. Substituting an ether to an ester bond at the 2‐position indicated that the number of carbon of the 2‐substituant seems more determinant than the nature of the linkage for the desensitizing process. Indeed, the 2‐ethoxy and the 2‐methoxy analogues were 87 and 5000 times less active than PAF‐acether respectively. The presence of methyl groups on the nitrogen base is also critical to desensitize platelets. The desensitizing potency of the tested phospholipids was always identical to their aggregating efficiency. It is suggested that these compounds activate cells through a common mechanism.

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