UCSC Genome Browser Gene Interaction Graph

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Gene interactions and pathways from curated databases and text-mining

IRF6 — PTK6

Text-mined interactions from Literome

Pedron et al., FEMS Immunol Med Microbiol 2000 : This particular response of BMC to LPS required the activation of protein tyrosine kinase and p38 MAP kinase
Ternisien et al., Thromb Haemost 1995 : As it has been established that LPS and PMA activate protein tyrosine kinase ( PTK ) in monocytes, we studied the role of PTK in LPS and PMA induction of TF by human blood monocytes ... Both LPS- and PMA induced TF activity was inhibited in a concentration dependent manner by the protein tyrosine kinase-specific inhibitors herbimycin A and genistein
Geng et al., J Immunol 1993 : Both PTK inhibitors also reduced the LPS activation of nuclear factor-kappa B (NF-kappa B), which is a transcription factor involved in the expression of cytokine genes such as IL-6 and TNF-alpha ... In summary, these findings suggest that protein kinase C and protein kinase A appear to have selective effects in the LPS induction of cytokines, whereas PTK is required for LPS induction of a broad spectrum of cytokines and NF-kappa B activation in monocytes
Meisel et al., Eur J Immunol 1996 : LPS induced TNF-alpha and IL-10 expression requires early activation of protein tyrosine kinases ( PTK )
Adamson et al., Cell adhesion and communication 1996 : However when PTK inhibitors were present during both agonist activation ( 2h ) and subsequent expression of E-selectin after removal of agonist ( 4h ) the PTK inhibitors resulted in a dose dependent reduction in both IL-1 alpha and LPS stimulated E-selectin expression ( IC50 = 50M ) ... Moreover when PTK inhibitors were only incubated with cells for the 4h after cytokine or LPS activation of cells, PTK inhibitors resulted in a more effective dose dependent reduction in IL-1 alpha or LPS stimulated E-selectin expression ( IC50 = 10M )
Liang et al., Biochem Biophys Res Commun 1997 : These results suggest that PTK is critical for hepatocyte NO synthesis, and DMSO inhibited NO synthesis may be associated with prevention of LPS/CM induced PTK activation in hepatocytes