Publication:
miR-29b Mediates NF-κB Signaling in KRAS-Induced Non-Small Cell Lung Cancers.

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cris.virtual.author-orcid0000-0001-5897-3647
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cris.virtualsource.author-orcid5641b881-1327-41ad-b043-e346c8e160cd
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datacite.rightsrestricted
dc.contributor.authorLangsch, Stephanie
dc.contributor.authorBaumgartner, Ulrich
dc.contributor.authorHaemmig, Stefan
dc.contributor.authorSchlup, Cornelia
dc.contributor.authorSchäfer, Stephan
dc.contributor.authorBerezowska, Sabina Anna
dc.contributor.authorRieger, Gregor
dc.contributor.authorDorn, Patrick
dc.contributor.authorTschan, Mario
dc.contributor.authorVassella, Erik
dc.date.accessioned2024-10-24T18:46:38Z
dc.date.available2024-10-24T18:46:38Z
dc.date.issued2016-07-15
dc.description.abstractA global understanding of miRNA function in EGFR signaling pathways may provide insights into improving the management of KRAS-mutant lung cancers, which remain relatively recalcitrant to treatment. To identify miRNAs implicated in EGFR signaling, we transduced bronchial epithelial BEAS-2B cells with retroviral vectors expressing KRAS(G12V) and monitored miRNA expression patterns by microarray analysis. Through this approach, we defined miR-29b as an important target for upregulation by mutant KRAS in non-small cell lung cancers. Cell biologic analyses showed that pharmacologic inhibition of EGFR or MEK was sufficient to reduce levels of miR-29b, while PI3K inhibition had no effect. In KRAS(G12V)-transduced BEAS-2B cells, introduction of anti-miR-29b constructs increased the sensitivity to apoptosis, arguing that miR-29b mediated apoptotic resistance conferred by mutant KRAS. Mechanistic investigations traced this effect to the ability of miR-29b to target TNFAIP3/A20, a negative regulator of NF-κB signaling. Accordingly, overexpression of an miR-29b-refractory isoform of TNFAIP3 restored NF-κB and extrinsic apoptosis, confirming that TNFAIP3 is a functionally relevant target of miR-29b. We also noted that miR-29b could confer sensitivity to intrinsic apoptosis triggered by exposure to cisplatin, a drug used widely in lung cancer treatment. Thus, miR-29b expression may tilt cells from extrinsic to intrinsic mechanisms of apoptosis. Overall, our results reveal a complexity in cancer for miR-29b, which can act as either an oncogene or tumor suppressor gene depending on signaling context. Cancer Res; 76(14); 4160-9. ©2016 AACR.
dc.description.numberOfPages10
dc.description.sponsorshipInstitut für Pathologie, Klinische Pathologie
dc.description.sponsorshipInstitut für Pathologie, Autopsie
dc.description.sponsorshipUniversitätsklinik für Thoraxchirurgie
dc.description.sponsorshipInstitut für Pathologie, Tumorpathologie
dc.description.sponsorshipInstitut für Pathologie
dc.identifier.doi10.7892/boris.92143
dc.identifier.pmid27199349
dc.identifier.publisherDOI10.1158/0008-5472.CAN-15-2580
dc.identifier.urihttps://boris-portal.unibe.ch/handle/20.500.12422/147461
dc.language.isoen
dc.publisherAmerican Association for Cancer Research AACR
dc.relation.ispartofCancer research
dc.relation.issn0008-5472
dc.relation.organizationDCD5A442BE2AE17DE0405C82790C4DE2
dc.relation.organizationDCD5A442C453E17DE0405C82790C4DE2
dc.relation.organizationDCD5A442BE57E17DE0405C82790C4DE2
dc.relation.organizationDCD5A442BAD7E17DE0405C82790C4DE2
dc.relation.organizationDCD5A442BC12E17DE0405C82790C4DE2
dc.relation.organizationDCD5A442BF89E17DE0405C82790C4DE2
dc.subject.ddc600 - Technology::610 - Medicine & health
dc.subject.ddc500 - Science::570 - Life sciences; biology
dc.titlemiR-29b Mediates NF-κB Signaling in KRAS-Induced Non-Small Cell Lung Cancers.
dc.typearticle
dspace.entity.typePublication
dspace.file.typetext
oaire.citation.endPage4169
oaire.citation.issue14
oaire.citation.startPage4160
oaire.citation.volume76
oairecerif.author.affiliationInstitut für Pathologie
oairecerif.author.affiliationInstitut für Pathologie, Tumorpathologie
oairecerif.author.affiliationInstitut für Pathologie, Tumorpathologie
oairecerif.author.affiliationInstitut für Pathologie
oairecerif.author.affiliationInstitut für Pathologie, Klinische Pathologie
oairecerif.author.affiliationInstitut für Pathologie, Klinische Pathologie
oairecerif.author.affiliationInstitut für Pathologie, Autopsie
oairecerif.author.affiliationUniversitätsklinik für Thoraxchirurgie
oairecerif.author.affiliationInstitut für Pathologie, Tumorpathologie
oairecerif.author.affiliationInstitut für Pathologie, Klinische Pathologie
oairecerif.author.affiliation2Departement Klinische Forschung, Forschungsgruppe Thoraxchirurgie
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unibe.description.ispublishedpub
unibe.eprints.legacyId92143
unibe.journal.abbrevTitleCANCER RES
unibe.refereedtrue
unibe.subtype.articlejournal

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