FRINK Linked Data Fragments server

Matches in SemOpenAlex for { <https://semopenalex.org/work/W2332494291> ?p ?o ?g. }

• W2332494291 abstract "Glioblastoma multiforme (GBM) tumors are the most deadly of brain tumors due to their diffuse infiltrative nature and tremendous heterogeneity. EGFR signaling is aberrantly activated in most GBM tumors, and clearly contributes to malignancy. However, targeting EGFR directly has been largely unsuccessful, for multiple reasons, including compensatory upregulation of other receptor tyrosine kinases (RTKs). Identifying and targeting key common signaling nodes downstream of multiple RTKs that drive invasion may be an effective therapeutic strategy. The Mixed Lineage Kinases (MLKs) are a family of MAP3Ks that activate multiple MAPK pathways, including c-Jun N-terminal kinase (JNK). Binding of GTP-bound Rac/Cdc42 activates MLK3. We investigated the role of MLK signaling on GBM cell migration and 3D spheroid invasion using an ATP-competitive pan-MLK inhibitor, as well as siRNA-mediated silencing of MLK3. Our data demonstrate that both MLK inhibition and MLK3 silencing dramatically reduce GBM migration and 3D invasion. EGF-induced GBM cell migration, as well as JNK activation, is blocked by a pan-MLK inhibitor and by MLK3 silencing. The Rac GEF, Dock180, is critical for GBM invasion. Based upon Drosophila genetics, the Dock180 homolog (MBC), a Rac GEF, acts upstream of Rac, the MLK homolog (slipper) and JNK. Therefore we hypothesized that Dock180 might be an upstream activator of MLKs. Our data show that Dock180 complexes with MLK3; and that ectopic expression of Dock180 activates both MLK3 and JNK in a Rac-dependent manner. Furthermore, silencing of either Dock180 or MLK3 leads to a similar reduction in EGF-induced JNK activation. Finally, ectopic expression of MLK3 (which leads to its auto-activation) is sufficient to rescue the defect in migration due to Dock180 silencing. Based upon these data, we propose that an EGFR-Dock180-Rac-MLK-JNK signaling axis drives GBM migration and 3D invasion, and that targeting MLKs may be a useful therapeutic approach for treating patients with GBM." @default.
• W2332494291 created "2016-06-24" @default.
• W2332494291 creator A5005627824 @default.
• W2332494291 creator A5009804879 @default.
• W2332494291 creator A5055520741 @default.
• W2332494291 date "2014-11-01" @default.
• W2332494291 modified "2023-09-26" @default.
• W2332494291 title "CS-22 * MIXED LINEAGE KINASE SIGNALING IS REQUIRED FOR GLIOBLASTOMA CELL MIGRATION AND INVASION" @default.
• W2332494291 doi "https://doi.org/10.1093/neuonc/nou242.22" @default.
• W2332494291 hasPubMedCentralId "https://www.ncbi.nlm.nih.gov/pmc/articles/4217979" @default.
• W2332494291 hasPublicationYear "2014" @default.
• W2332494291 type Work @default.
• W2332494291 sameAs 2332494291 @default.
• W2332494291 citedByCount "0" @default.
• W2332494291 crossrefType "journal-article" @default.
• W2332494291 hasAuthorship W2332494291A5005627824 @default.
• W2332494291 hasAuthorship W2332494291A5009804879 @default.
• W2332494291 hasAuthorship W2332494291A5055520741 @default.
• W2332494291 hasBestOaLocation W23324942912 @default.
• W2332494291 hasConcept C101544691 @default.
• W2332494291 hasConcept C104317684 @default.
• W2332494291 hasConcept C119056186 @default.
• W2332494291 hasConcept C137361374 @default.
• W2332494291 hasConcept C2779717556 @default.
• W2332494291 hasConcept C2909331102 @default.
• W2332494291 hasConcept C42362537 @default.
• W2332494291 hasConcept C502942594 @default.
• W2332494291 hasConcept C55493867 @default.
• W2332494291 hasConcept C57074206 @default.
• W2332494291 hasConcept C62478195 @default.
• W2332494291 hasConcept C86803240 @default.
• W2332494291 hasConcept C95444343 @default.
• W2332494291 hasConceptScore W2332494291C101544691 @default.
• W2332494291 hasConceptScore W2332494291C104317684 @default.
• W2332494291 hasConceptScore W2332494291C119056186 @default.
• W2332494291 hasConceptScore W2332494291C137361374 @default.
• W2332494291 hasConceptScore W2332494291C2779717556 @default.
• W2332494291 hasConceptScore W2332494291C2909331102 @default.
• W2332494291 hasConceptScore W2332494291C42362537 @default.
• W2332494291 hasConceptScore W2332494291C502942594 @default.
• W2332494291 hasConceptScore W2332494291C55493867 @default.
• W2332494291 hasConceptScore W2332494291C57074206 @default.
• W2332494291 hasConceptScore W2332494291C62478195 @default.
• W2332494291 hasConceptScore W2332494291C86803240 @default.
• W2332494291 hasConceptScore W2332494291C95444343 @default.
• W2332494291 hasLocation W23324942911 @default.
• W2332494291 hasLocation W23324942912 @default.
• W2332494291 hasOpenAccess W2332494291 @default.
• W2332494291 hasPrimaryLocation W23324942911 @default.
• W2332494291 hasRelatedWork W1150630736 @default.
• W2332494291 hasRelatedWork W1977223089 @default.
• W2332494291 hasRelatedWork W1996816592 @default.
• W2332494291 hasRelatedWork W2027623923 @default.
• W2332494291 hasRelatedWork W2037274964 @default.
• W2332494291 hasRelatedWork W2050454735 @default.
• W2332494291 hasRelatedWork W2051257252 @default.
• W2332494291 hasRelatedWork W2060776420 @default.
• W2332494291 hasRelatedWork W2084221469 @default.
• W2332494291 hasRelatedWork W2101203152 @default.
• W2332494291 hasRelatedWork W2117139777 @default.
• W2332494291 hasRelatedWork W2118020290 @default.
• W2332494291 hasRelatedWork W2118462075 @default.
• W2332494291 hasRelatedWork W2122074931 @default.
• W2332494291 hasRelatedWork W2133505501 @default.
• W2332494291 hasRelatedWork W2137047140 @default.
• W2332494291 hasRelatedWork W2146878112 @default.
• W2332494291 hasRelatedWork W2222820521 @default.
• W2332494291 hasRelatedWork W2313453036 @default.
• W2332494291 hasRelatedWork W2321021356 @default.
• W2332494291 isParatext "false" @default.
• W2332494291 isRetracted "false" @default.
• W2332494291 magId "2332494291" @default.
• W2332494291 workType "article" @default.