Jx. Peng et al., ACTIVATION OF AP-1 BY OKADAIC ACID IN MOUSE KERATINOCYTES ASSOCIATED WITH HYPERPHOSPHORYLATION OF C-JUN, Molecular carcinogenesis, 18(1), 1997, pp. 37-43
Okadaic acid (OA), a specific inhibitor of protein phosphatases 1 and
2A, is also a potent mouse skin tumor promoter. The effects of OA on r
egulation of c-jun/activator protein-1 (AP-1) transcriptional activati
on were investigated in mouse keratinocytes. AP-1 DNA binding to the j
un 12-O-tetradecanoylphorbol-13-acetate-response element (TGACATCA) as
determined by gel shift analysis was strongly induced by OA (100 ng/m
L) at 6 and 12 h. Preincubation of nuclear extracts with anti-c-jun an
tibody demonstrated that c-jun was a major component of the DNA-bound
AP-1 complex induced by OA in 308 cells. Transfection of a c-jun promo
ter-reporter construct demonstrated that AP-1 transactivation was indu
ced by OA. The mRNA level of the c-jun proto-oncogene was dramatically
increased by 6 and 12 h of OA treatment. Furthermore, a significant i
nduction of c-jun protein was stimulated by 6 and 12 h of OA treatment
. Upon further analysis, it was found that OA induced a significant ac
cumulation of Ser 73-phosphorylated c-jun protein in 308 cells. In sum
mary, our data suggest that skin tumor promotion by OA is due at least
in part to increased AP-1 DNA binding and transactivation mediated by
c-jun hyperphosphorylation. (C) 1997 Wiley-Liss, Inc.