1997
DOI: 10.1038/sj.onc.1201403
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Effects of the inhibition of p38/RK MAP kinase on induction of five fos and jun genes by diverse stimuli

Abstract: The ERK, JNK/SAPK and p38/RK MAP kinase subtypes are di erentially activated by physiological, pharmacological and stress stimuli; all three subtypes are implicated in immediate-early (IE) gene induction by these agents. Here, we have asked whether inhibition of a single MAP kinase subtype under these conditions would generally alter induction of several IE genes in a similar way or whether this would di erentially up-and down-regulate particular IE genes, an issue which bears on the question of whether indivi… Show more

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Cited by 95 publications
(81 citation statements)
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“…This increased AP-1 activity correlated with activation of the MAP kinases ERK-1/ 2, JNK and p38 MAPK, and ERK-1/2 activation appeared to play a critical role in okadaic acid mediated e ects on this transcription factor complex (Rosenberger et al, 1999). Various other studies implying p38 MAP kinase in AP-1 regulation (Hazzalin et al, 1996(Hazzalin et al, , 1997 suggest that p38 MAP kinase may also be involved in okadaic acid induced AP-1 activation. To test this hypothesis we used SB 203580, a pyridinyl-imidazole compound described as speci®c inhibitor of this enzyme (Lee et al, 1994;Cuenda et al, 1995), in an attempt to block p38 MAP kinase activation.…”
Section: Resultsmentioning
confidence: 72%
See 1 more Smart Citation
“…This increased AP-1 activity correlated with activation of the MAP kinases ERK-1/ 2, JNK and p38 MAPK, and ERK-1/2 activation appeared to play a critical role in okadaic acid mediated e ects on this transcription factor complex (Rosenberger et al, 1999). Various other studies implying p38 MAP kinase in AP-1 regulation (Hazzalin et al, 1996(Hazzalin et al, , 1997 suggest that p38 MAP kinase may also be involved in okadaic acid induced AP-1 activation. To test this hypothesis we used SB 203580, a pyridinyl-imidazole compound described as speci®c inhibitor of this enzyme (Lee et al, 1994;Cuenda et al, 1995), in an attempt to block p38 MAP kinase activation.…”
Section: Resultsmentioning
confidence: 72%
“…This hypothesis is consistent with our preliminary ®nding that while SB 203580 decreases MAPKAP kinase-2 phosphorylation it increases p38 MAP kinase mediated phosphorylation of Elk-1 (data not shown). Further evidence comes from a report by Hazzalin et al (1997) who documented elevated activity of the p38 MAP kinase activator MKK6 without an increase in MAKAP kinase-2 phosphorylation.…”
Section: Discussionmentioning
confidence: 99%
“…Thus, an explanation for this effect of SB203580 might be provided by a potential feedback between kinase pathways, so that inhibition of p38 MAP kinase activity by SB203580 might result in the up-regulation of another kinase activity which would positively regulate IL-1b release. Such feedback is already demonstrated for MKK6, an upstream activator of p38 MAP kinase, whose activity is potentiated by SB-like compounds (Hazzalin et al 1997). Recently, p38 MAP kinase was found to down-regulate ERK activity by direct protein-protein interaction (Hong Zhang et al 2001), and additionally, monocytes treated with the MEK inhibitor U0126 failed to release IL-1b, TNF-a, IL-8 and prostaglandin E 2 (PGE 2 ), indicating the involvement of the ERK pathway in cytokine and PG synthesis and/or release (Scherle et al 1998).…”
Section: Discussionmentioning
confidence: 75%
“…The ®nding that c-Raf is inhibited by SB 203580 at micromolar concentrations was surprising because we have reported previously that the activation of MAPK1 and MAPK2 by NGF in rat PC12 cells , by EGF or IGF-1 in human KB cells Gould et al, 1995), or by EGF or phorbol esters in mouse C3H 10T1/2 cells (Hazzalin et al, 1997), is not inhibited by SB 203580. In the present study we con®rmed this result for EGFstimulated Swiss 3T3 cells ( Figure 2) and IGF-1 stimulated rat L6 myotubes (data not shown).…”
Section: Failure Of Sb 203580 To Prevent the Activation Of Mkk1 Or Mamentioning
confidence: 96%
“…SB 203580 does not a ect the activation of the classical MAP kinase cascade by a variety of agonists Gould et al, 1995;Hazzalin et al, 1997). However, the protein kinase that is thought to lie at the head of this cascade, the proto-oncogene cRaf, contains threonine at the position equivalent to Thr 106 of SAPK2a/p38a.…”
Section: Introductionmentioning
confidence: 98%