INVOLVEMENT OF PROTEIN-KINASE-C IN THE INTERLEUKIN-1 ALPHA-INDUCED GENE-EXPRESSION OF MATRIX METALLOPROTEINASES AND TISSUE INHIBITOR-1 OF METALLOPROTEINASES (TIMP-1) IN HUMAN UTERINE CERVICAL FIBROBLASTS
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TAKAHASHI, S
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机构:TOKYO COLL PHARM, DEPT BIOCHEM, HACHIOJI, TOKYO 19203, JAPAN
TAKAHASHI, S
SATO, T
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机构:TOKYO COLL PHARM, DEPT BIOCHEM, HACHIOJI, TOKYO 19203, JAPAN
SATO, T
ITO, A
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机构:TOKYO COLL PHARM, DEPT BIOCHEM, HACHIOJI, TOKYO 19203, JAPAN
ITO, A
OJIMA, Y
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机构:TOKYO COLL PHARM, DEPT BIOCHEM, HACHIOJI, TOKYO 19203, JAPAN
OJIMA, Y
HOSONO, T
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HOSONO, T
NAGASE, H
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NAGASE, H
MORI, Y
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MORI, Y
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[1] TOKYO COLL PHARM, DEPT BIOCHEM, HACHIOJI, TOKYO 19203, JAPAN
[2] UNIV KANSAS, MED CTR, DEPT BIOCHEM & MOLEC BIOL, KANSAS CITY, KS 66160 USA
The role of protein kinase C in the interleukin 1 (IL-1)-mediated production of pro-matrix metalloproteinases (proMMPs) and tissue inhibitor-1 of metalloproteinases (TIMP-1) in human uterine cervical fibro-blasts has been investigated. IL-1 and a protein kinase C activator, 12-O-tetradecanoylphorbol 13-acetate (TPA) augmented the production of proMMP-1 (interstitial procollagenase), proMMP-3 (prostromelysin-1) and TIMP-1, but their effects were inhibited by the protein kinase C inhibitors 1-(5-isoquinolinesulfonyl)-2-methylpiperazine dihydrochloride (H-7) and staurosporine in a dose-dependent manner. The suppressive effect of H-7 and staurosporine on the IL-1-induced production of proMMPs-1 and -3 and TIMP-1 resulted from the decrease in the steady-state levels of their mRNAs. When protein kinase C was down-regulated by treating the cells with a high level of TPA, the inductive effect of IL-1 upon proMMP-3 production was reduced considerably. These results indicate that protein kinase C mediates the IL-1-induced production of proMMPs-1 and -3 and TIMP-1 at the pretranslational level in human uterine cervical fibroblasts. On the other hand, neither IL-1 nor TPA modulated the production of proMMP-2 (progelatinase A). Both IL-1 and TPA also accelerated the production of prostaglandin E2 (PGE2) by cervical fibroblasts. However, the treatment of the cells with staurosporine in the presence of IL-1 or TPA further augmented PGE2 synthesis, suggesting that the increased synthesis of PGE2 by IL-1 treatment is mediated via signalling pathways distinct from those of proMMPs-1 and -3 and TIMP-1.