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Query: UMLS:C0001511 (
Adhesion
)
5,955
document(s) hit in 31,850,051 MEDLINE articles (0.00 seconds)
Cell adhesion-dependent activation of ERK1/2 has been linked functionally to focal adhesion dynamics. We previously reported that in adherent vascular smooth muscle (VSM) cells,
CaMKII
mediates ERK1/2 activation in response to Ca(2+)-mobilizing stimuli. In the present study, we tested whether
CaMKII
regulates ERK1/2 signaling in response to VSM cell adhesion. Using an antibody that specifically recognizes
CaMKII
autophosphorylated on Thr(287), we determined that
CaMKII
is rapidly activated (within 1 min) after the adherence of cells on multiple ECM substrates. Activation of
CaMKII
on fibronectin was unaffected in cells overexpressing focal adhesion kinase (FAK)-related nonkinase (FRNK), an endogenous inhibitor of FAK. Furthermore,
CaMKII
was rapidly and robustly activated in VSM cells plated on poly-l-lysine. These results suggest that adhesion-dependent
CaMKII
activation is integrin independent.
Adhesion
-dependent FAK activation on fibronectin was not affected in cells treated with the selective
CaMKII
inhibitor KN-93 (30 muM) or in cells in which the expression of
CaMKII
with small interfering RNA (siRNA) was suppressed, although tyrosine phosphorylation of paxillin was inhibited in
CaMKII
-delta(2)-suppressed cells. Sustained ERK1/2 activation that was dependent on FAK activation (inhibited by FRNK) was also attenuated by
CaMKII
inhibition or siRNA-mediated gene silencing. Rapid ERK1/2 activation that preceded FAK and paxillin activation was detected upon VSM cell adhesion to poly-l-lysine, and this response was inhibited by
CaMKII
gene silencing. These results indicate that integrin-independent
CaMKII
activation is an early signal during VSM cell adhesion that positively modulates ERK1/2 signaling through FAK-dependent and FAK-independent mechanisms.
...
PMID:Adhesion-dependent activation of CaMKII and regulation of ERK activation in vascular smooth muscle. 1594 10
