Lk. Lockhart et al., Evidence for a role for phospholipase C, but not phospholipase A(2), in platelet activation in response to low concentrations of collagen, THROMB HAEM, 85(5), 2001, pp. 882-889
The release of arachidonic acid is a key component in platelet activation i
n response to low concentrations (1-20 mug/ml) of collagen. The precise mec
hanism remains elusive although a variety of pathways have been implicated.
In the present study the effects of inhibitors of several potentially key
enzymes in these pathways have been examined. Collagen (1-10 mug/ml) caused
maximal platelet aggregation which was accompanied by the release of arach
idonic acid, the synthesis of thromboxane A(2), and p38(MAPK) phosphorylati
on. Preincubation with the dual cyclooxygenase/lipoxygenase inhibitor BW755
C inhibited aggregation and thromboxane production, and reduced p38(MAPK) p
hosphorylation. A phospholipase C inhibitor, U73122, blocked collagen-induc
ed aggregation and reduced arachidonic acid release, thromboxane synthesis
and p38(MAPK) phosphorylation. Pretreatment with a cytosolic phospholipase
A(2) inhibitor, AACOCF(3), blocked collagen-induced aggregation, reduced th
e levels of thromboxane formation and p38(MAPK) phosphorylation but had no
significant effect on arachidonic acid release. In contrast inhibition of P
KC by Ro31-8220 inhibited collagen-induced aggregation, did not affect p38(
MAPK) phosphorylation hut significantly potentiated arachidonic acid releas
e and thromboxane formation. Collagen caused the tyrosine phosphorylation o
f phospholipase C gamma2 which was inhibited by pretreatment with U73122, u
naffected by AACOCF(3) and enhanced by Ro31-8220. These results suggest tha
t cytosolic phospholipase A(2) plays no role in the arachidonic acid releas
e in response to collagen. In contrast, the data are consistent with phosph
olipase C gamma2 playing a role in an intricately controlled pathway, or mu
ltiple pathways, mediating the release of arachidonic acid in collagen-stim
ulated platelets.