@article{ajmbr2015353,
author={Haddad, John J},
title={The Irreversible Inhibition of the MAPK<SUP>p38</SUP> Pathway Downregulates LPS-augmented Release of Interleukin-Related Inflammatory Cytokines (IL-1&#946;, IL-6): Immune Surveillance Unraveling I&#954;B-¦Á/NF-&#954;B Phosphorylation State-independent Mechanism <i>in vitro</i>},
journal={American Journal of Medical and Biological Research},
volume={3},
number={5},
pages={133--138},
year={2015},
url={http://pubs.sciepub.com/ajmbr/3/5/3},
issn={2328-4099},
abstract={<b>Background:</b> The participation of signaling pathways involving the mitogen-activated protein kinases (MAPKs) in regulating the inflammatory response characterized by the release of cytokines is not well established in the alveolar epithelium. We have previously examined the effect of MAPK<SUP>p38</SUP> blockade on the <i>in vitro</i> release of TNF-¦Á, indicating the likely involvement of other pro-inflammatory cytokines. <b>Methods:</b> This study investigated the selective inhibition of MAPK<SUP>p38</SUP> in modulating the release of interleukin-related inflammatory cytokines, including IL-1&#946; and IL-6. LPS-mediated release of cytokines is closely associated with the blockade of MAPK by the compound SB203580, an irreversible and selective inhibitor of MAPK<SUP>p38</SUP>, independent of MAPK<SUP>ERK (p42/p44) </SUP>and MAPK<SUP>JNK</SUP>. <b>Results:</b> Pre-treatment with ascending concentrations of SB203580 (0.1 ¨C 100 &#956;M) prior to LPS administration downregulated/attenuated the release of IL-1&#946;, IL-6 and TNF-¦Á in a dose-dependent and dose-independent manners. Furthermore, unraveling the immune molecular pathways likely involved with MAPK<SUP>p38</SUP>-mediated secretion of cytokines revealed that SB203580 increased I&#954;B-¦Á phosphorylation, where I&#954;B-¦Á is considered the main cytosolic inhibitor of the transcription factor involved with regulating the processes of cellular inflammation, NF-&#954;B. This upregulation of the phosphorylation status of I&#954;B-¦Á was accompanied by downregulating the cytosolic accumulation of the non-phosphorylated form of I&#954;B-¦Á, indicating normal nuclear translocation of the associated transcription factor. <b>Conclusions:</b> These results show that MAPK<SUP>p38</SUP> is required, at least in part, for the release of inflammatory cytokines induced by LPS, a mechanism that is independent of the phosphorylation of I&#954;B-¦Á. In addition, the MAPK<SUP>p38</SUP>-dependent release of cytokines seemingly does not require the activation of the NF-&#954;B pathway.},
doi={10.12691/ajmbr-3-5-3}
publisher={Science and Education Publishing}
}