| |
[摘要]:We have demonstrated that LPA (lysophosphatidic acid)induced IL (interleukin)-8 secretion was partly mediated via transactivation of EGFR [EGF (epidermal growth factor) receptor] in HBEpCs (human bronchial epithelial primary cells). The present study provides evidence that LPA-induced transactivation of EGFR regulates COX (cyclo-oxygenase)-2 expression and PGE2 [PG (prostaglandin) E,] release through the transcriptional factor, C/EBPP (CCAAT/enhancer-binding protein P), in HBEpCs. Treatment with LPA (1 mu M) stimulated COX-2 mRNA and protein expression and PGE2 release via G(alpha i)-coupled LPARs (LPA receptors). Pretreatment with inhibitors of NF-kappa B (nuclear factor-kappa B), JNK (Jun N-terminal kinase), or down-regulation of c-Jun or C/EBP beta with specific siRNA (small interference RNA) attenuated LPA-induced COX-2 expression. Downregulation of EGFR by siRNA or pretreatment with the EGFR tyrosine kinase inhibitor, AG 1478, partly attenuated LPA-induced COX-2 expression and phosphorylation of C/EBPP; however, neither of these factors had an effect on the NF-kappa B and JNK pathways. Furthermore, LPA-induced EGFR transactivation, phosphorylation of C/EBP beta and COX-2 expression were attenuated by overexpression of a catalytically inactive mutant of PLD2 [PLD (phospholipase D) 2], PLD2-K758R, or by addition of myristoylated PKC zeta [PKC (protein kinase Q] peptide pseudosubstrate. Overexpression of the PLD2-K758R mutant also attenuated LPA-induced phosphorylation and activation of PKC zeta. These results demonstrate that LPA induces COX-2 expression and PGE2 production through EGFR transactivation-independent activation of transcriptional factors NF-kappa B and c-Jun, and EGFR trans activation-dependent activation of C/EBP beta in HBEpCs. Since COX-2 and PGE2 have been shown to be anti-inflammatory in airway inflammation, the present data suggest a modulating and protective role of LPA in regulating innate immunity and remodelling of the airways. |
|
