SemOpenAlex |

SemOpenAlex

Matches in SemOpenAlex for { <https://semopenalex.org/work/W4361946175> ?p ?o ?g. }

Showing items 1 to 78 of 78 with 100 items per page.

W4361946175 abstract "<div>AbstractPurpose: Notch1 deregulation is assuming a focal role in T-cell acute lymphoblastic leukemia (T-ALL). Despite tremendous advances in our understanding of Notch1 transcriptional programs, the mechanisms by which Notch1 stability and turnover are regulated remain obscure. The goal of the current study is to identify intracellular Notch1 (ICN1, the activated form of Notch1) binding partner(s) regulating its stability and activity.Experimental Design: We employed immunoaffinity purification to identify ICN1-associating partner(s) and used coimmunoprecipitation to verify the endogenous protein interaction. Pharmacologic or short hairpin RNA–mediated inhibition was applied in loss-of-function assays to assess the role of tentative binding partner(s) in modulating ICN1 protein stability as well as affecting T-ALL cell expansion in vitro and in vivo. Mechanistic analysis involved protein degradation and polyubiquitination assays.Results: We identify the Hsp90 chaperone as a direct ICN1-binding partner essential for its stabilization and transcriptional activity. T-ALL cells exhibit constitutive endogenous ICN1–Hsp90 interaction and Hsp90 depletion markedly decreases ICN1 levels. The Hsp90-associated E3 ubiquitin ligase Stub1 mediates the ensuring proteasome-dependent ICN1 degradation. Administration of 17-AAG or PU-H71, two distinct Hsp90 inhibitors, depletes ICN1, inhibits T-ALL cell proliferation, and triggers dramatic apoptotic cell death. Systemic treatment with PU-H71 reduces ICN1 expression and profoundly inhibits murine T-ALL allografts as well as human T-ALL xenografts.Conclusions: Our findings demonstrate Hsp90 blockade leads to ICN1 destabilization, providing an alternative strategy to antagonize oncogenic Notch1 signaling with Hsp90-selective inhibitors. Clin Cancer Res; 23(14); 3834–46. ©2017 AACR.</div>" @default.
W4361946175 created "2023-04-05" @default.
W4361946175 creator A5024686608 @default.
W4361946175 creator A5027639672 @default.
W4361946175 creator A5028904438 @default.
W4361946175 creator A5031557150 @default.
W4361946175 creator A5033263569 @default.
W4361946175 creator A5053322275 @default.
W4361946175 creator A5060052615 @default.
W4361946175 creator A5071458554 @default.
W4361946175 creator A5077759715 @default.
W4361946175 creator A5080015407 @default.
W4361946175 creator A5086894006 @default.
W4361946175 creator A5086942958 @default.
W4361946175 date "2023-03-31" @default.
W4361946175 modified "2023-09-26" @default.
W4361946175 title "Data from Stabilization of Notch1 by the Hsp90 Chaperone is Crucial for T-Cell Leukemogenesis" @default.
W4361946175 doi "https://doi.org/10.1158/1078-0432.c.6526175" @default.
W4361946175 hasPublicationYear "2023" @default.
W4361946175 type Work @default.
W4361946175 citedByCount "0" @default.
W4361946175 crossrefType "posted-content" @default.
W4361946175 hasAuthorship W4361946175A5024686608 @default.
W4361946175 hasAuthorship W4361946175A5027639672 @default.
W4361946175 hasAuthorship W4361946175A5028904438 @default.
W4361946175 hasAuthorship W4361946175A5031557150 @default.
W4361946175 hasAuthorship W4361946175A5033263569 @default.
W4361946175 hasAuthorship W4361946175A5053322275 @default.
W4361946175 hasAuthorship W4361946175A5060052615 @default.
W4361946175 hasAuthorship W4361946175A5071458554 @default.
W4361946175 hasAuthorship W4361946175A5077759715 @default.
W4361946175 hasAuthorship W4361946175A5080015407 @default.
W4361946175 hasAuthorship W4361946175A5086894006 @default.
W4361946175 hasAuthorship W4361946175A5086942958 @default.
W4361946175 hasConcept C104317684 @default.
W4361946175 hasConcept C134459356 @default.
W4361946175 hasConcept C16613235 @default.
W4361946175 hasConcept C173396325 @default.
W4361946175 hasConcept C185592680 @default.
W4361946175 hasConcept C190232843 @default.
W4361946175 hasConcept C190283241 @default.
W4361946175 hasConcept C205260736 @default.
W4361946175 hasConcept C25602115 @default.
W4361946175 hasConcept C2775932338 @default.
W4361946175 hasConcept C502942594 @default.
W4361946175 hasConcept C55493867 @default.
W4361946175 hasConcept C62112901 @default.
W4361946175 hasConcept C71924100 @default.
W4361946175 hasConceptScore W4361946175C104317684 @default.
W4361946175 hasConceptScore W4361946175C134459356 @default.
W4361946175 hasConceptScore W4361946175C16613235 @default.
W4361946175 hasConceptScore W4361946175C173396325 @default.
W4361946175 hasConceptScore W4361946175C185592680 @default.
W4361946175 hasConceptScore W4361946175C190232843 @default.
W4361946175 hasConceptScore W4361946175C190283241 @default.
W4361946175 hasConceptScore W4361946175C205260736 @default.
W4361946175 hasConceptScore W4361946175C25602115 @default.
W4361946175 hasConceptScore W4361946175C2775932338 @default.
W4361946175 hasConceptScore W4361946175C502942594 @default.
W4361946175 hasConceptScore W4361946175C55493867 @default.
W4361946175 hasConceptScore W4361946175C62112901 @default.
W4361946175 hasConceptScore W4361946175C71924100 @default.
W4361946175 hasLocation W43619461751 @default.
W4361946175 hasOpenAccess W4361946175 @default.
W4361946175 hasPrimaryLocation W43619461751 @default.
W4361946175 hasRelatedWork W1964312498 @default.
W4361946175 hasRelatedWork W2032264124 @default.
W4361946175 hasRelatedWork W2087632584 @default.
W4361946175 hasRelatedWork W2116511323 @default.
W4361946175 hasRelatedWork W2139095751 @default.
W4361946175 hasRelatedWork W2610003092 @default.
W4361946175 hasRelatedWork W4239805490 @default.
W4361946175 hasRelatedWork W4299445875 @default.
W4361946175 hasRelatedWork W4319881081 @default.
W4361946175 hasRelatedWork W2024244776 @default.
W4361946175 isParatext "false" @default.
W4361946175 isRetracted "false" @default.
W4361946175 workType "article" @default.