| Journal of Leukocyte Biology: An Official Publication of the Reticuloendothelial Society | |
| A novel p38‐MAPK signaling axis modulates neutrophil biology in head and neck cancer | |
| 关键词: p27; CREB; inflammation; CCL4; MMP9; | |
| DOI : 10.1189/jlb.0411193 | |
| 学科分类:生理学 | |
| 来源: Federation of American Societies for Experimental Biology | |
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【 摘 要 】
Neutrophilsareemergingasimportantmediatorsincancerprogression.RecentstudiesassociatedneutrophilswithpoorclinicaloutcomeofHNCpatientsandshowedthatHNCinducesrecruitment,survival,andreleaseofproinflammatoryfactorsbyneutrophilsinvitro.ThemolecularmechanismsthroughwhichHNCandothercancersmodulateneutrophilbiologyarecurrentlyunknown.Toexplorethesemechanisms,weusedaninvitrosystemthatmodelstheinteractionbetweenhumanHNCcellsandneutrophilsorneutrophilic‐differentiatedHL‐60cells,respectively.WeshowthatHNC‐derivedfactorsactivatep38‐MAPKinneutrophils,whichpartlypromotesneutrophilsurvival,butnotneutrophilrecruitmentandmotility.Mostimportantly,HNC‐inducedp38‐MAPKactivationstronglystimulatesthereleaseofCCL4,CXCL8,andMMP9byneutrophils.WeidentifyCREBandinterestingly,p27phosphorylatedatT198asdownstreammembersoftheHNC‐inducedp38‐MAPKsignalingcascade.UsingsiRNAtechnology,wedemonstratethatp27andCREBmediatethereleaseofCCL4andCXCL8andthatCREB,additionally,mediatesthereleaseofMMP9.Thesedataunravelnovelmolecularmechanismsinvolvedinregulationofneutrophilproinflammatoryfunctions.OurstudiesonhumanHNCtissuesindicatethattumor‐infiltratingneutrophilsmightbeamajorsourceofCCL4andparticularly,MMP9incancerpatients.Thus,ourfindingsprovidenovel,mechanisticinsightsrelevantforthepathophysiologyofHNCandpossibly,othertypesofcanceraswell...
【 授权许可】
CC BY
【 预 览 】
| Files | Size | Format | View |
|---|---|---|---|
| RO201904043422185ZK.pdf | 1757KB |  download |
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