Fkhr1
Regulation of
the forkhead domain transcription factors by PDGF has
not been studied. In this report, we investigated the role of PDGF-induced Akt in regulating forkhead domain
protein FKHRL1 in glomerular mesangial
cells. PDGF increased phosphorylation of FKHRL1 in a
time- and PI 3 kinase-dependent manner. Expression of
dominant negative Akt by adenovirus-mediated gene
transfer blocked PDGF-induced FKHRL1 phosphorylation.
PDGF inhibited transcription of a forkhead DNA
binding element-driven reporter gene. This inhibition was mimicked by
constitutively active myristoylated Akt. Moreover, FKHR1-mediated transcription of the reporter
gene was completely attenuated by both PDGF and Myr-Akt.
One of the targets of forkhead transcription factors
is the proapoptotic Fas ligand (FasL) gene. PDGF, as well as Myr-Akt, inhibited
transcription of FasL. In contrast, inhibition
of PI 3 kinase and dominant negative Akt increased FasL gene
transcription, suggesting that suppression of PI 3 kinase/Akt
signalling may induce apoptosis in mesangial cells via upregulation
of FasL expression. However, expression of dominant
negative Akt by adenovirus did not induce apoptosis
in mesangial cells, suggesting that Akt-independent antiapoptotic
mechanisms also exist. Together, our data demonstrate for the first time that
PDGF inactivates forkhead domain transcription factor
by Akt-dependent phosphorylation
and that suppression of Akt signalling
is not sufficient to induce apoptosis in mesangial
cells.
PMID: 12464387 [PubMed - indexed for MEDLINE]