SemOpenAlex |

SemOpenAlex

Matches in SemOpenAlex for { <https://semopenalex.org/work/W2286232018> ?p ?o ?g. }

Showing items 1 to 75 of 75 with 100 items per page.

W2286232018 abstract "Histone deacetylases (HDACs) are enzymes involved in the remodeling of chromatin. In recent years, inhibition of HDACs has emerged as a potential strategy to reverse aberrant epigenetic changes associated with cancer. In fact, HDAC inhibitors (HDACi) promote apoptosis, induce cell cycle arrest and differentiation of tumor cells, by mechanisms which remain in part unknown. T-cell acute lymphoblastic leukemia (T-ALL) is a pediatric malignancy characterized by clonal expansion of lymphoid progenitors. Although the majority of pediatric T-ALL patients can be cured by current protocols, about one fourth of patients has chemotherapy-resistant disease or relapse after therapy and novel therapeutic approaches are required. In our study, we analyzed the effects of HDACi on seven transcription factors important in T-ALL pathogenesis (NOTCH1, NOTCH3, c-MYB, TAL1, TLX1, TLX3 and LMO2) using both established T-ALL cell lines and patient-derived T-ALL xenografts previously obtained in our laboratory. In particular, we focused on transcription factors that define specific T-ALL subgroups (TAL/LMO, TLX1, TLX3) and we included members of the Notch family (NOTCH1 and NOTCH3) and c-MYB in view of their transversal role in T-ALL. In vitro analysis highlighted transcriptional down-regulation of C-MYB and TAL1, a post-translation regulation of NOTCH1 and NOTCH3 and the regulation of the transcriptional activity of TLX1 and TLX3 following HDAC inhibition. These biochemical effects were linked to increased apoptosis and impaired proliferation both in T-ALL cell lines and patients-derived cells, partially dependent on NOTCH1 and NOTCH3. We next investigated the in vivo effects of an HDACi in T-ALL xenografts belonging to specific T-ALL subgroups. Interestingly, PD-TALL8 (TLX1) and PD-TALL16 (TLX3) had better response to treatment compared to PD-TALL12 and PD-TALL9 (TAL/LMO). In fact, the HDACi dramatically decreased leukemic cells infiltrating the spleen and the bone marrow in TLX-driven xenografts, whereas this drug had modest or minimal effects on TAL/LMO xenografts. Taken together, these results identify TLX1 and TLX3 T-ALL subgroups as potential candidates for therapeutic treatment with HDACi." @default.
W2286232018 created "2016-06-24" @default.
W2286232018 creator A5074275562 @default.
W2286232018 date "2014-01-30" @default.
W2286232018 modified "2023-09-24" @default.
W2286232018 title "HDAC INHIBITORS TARGET TRANSCRIPTION FACTORS DEREGULATED IN T-ACUTE LYMPHOBLASTIC LEUKAEMIA" @default.
W2286232018 hasPublicationYear "2014" @default.
W2286232018 type Work @default.
W2286232018 sameAs 2286232018 @default.
W2286232018 citedByCount "0" @default.
W2286232018 crossrefType "journal-article" @default.
W2286232018 hasAuthorship W2286232018A5074275562 @default.
W2286232018 hasConcept C104317684 @default.
W2286232018 hasConcept C150194340 @default.
W2286232018 hasConcept C161879069 @default.
W2286232018 hasConcept C167227067 @default.
W2286232018 hasConcept C190283241 @default.
W2286232018 hasConcept C190727270 @default.
W2286232018 hasConcept C2780737395 @default.
W2286232018 hasConcept C41091548 @default.
W2286232018 hasConcept C502942594 @default.
W2286232018 hasConcept C54355233 @default.
W2286232018 hasConcept C62478195 @default.
W2286232018 hasConcept C62794011 @default.
W2286232018 hasConcept C64927066 @default.
W2286232018 hasConcept C71924100 @default.
W2286232018 hasConcept C83640560 @default.
W2286232018 hasConcept C86339819 @default.
W2286232018 hasConcept C86803240 @default.
W2286232018 hasConcept C95444343 @default.
W2286232018 hasConceptScore W2286232018C104317684 @default.
W2286232018 hasConceptScore W2286232018C150194340 @default.
W2286232018 hasConceptScore W2286232018C161879069 @default.
W2286232018 hasConceptScore W2286232018C167227067 @default.
W2286232018 hasConceptScore W2286232018C190283241 @default.
W2286232018 hasConceptScore W2286232018C190727270 @default.
W2286232018 hasConceptScore W2286232018C2780737395 @default.
W2286232018 hasConceptScore W2286232018C41091548 @default.
W2286232018 hasConceptScore W2286232018C502942594 @default.
W2286232018 hasConceptScore W2286232018C54355233 @default.
W2286232018 hasConceptScore W2286232018C62478195 @default.
W2286232018 hasConceptScore W2286232018C62794011 @default.
W2286232018 hasConceptScore W2286232018C64927066 @default.
W2286232018 hasConceptScore W2286232018C71924100 @default.
W2286232018 hasConceptScore W2286232018C83640560 @default.
W2286232018 hasConceptScore W2286232018C86339819 @default.
W2286232018 hasConceptScore W2286232018C86803240 @default.
W2286232018 hasConceptScore W2286232018C95444343 @default.
W2286232018 hasLocation W22862320181 @default.
W2286232018 hasOpenAccess W2286232018 @default.
W2286232018 hasPrimaryLocation W22862320181 @default.
W2286232018 hasRelatedWork W1476000644 @default.
W2286232018 hasRelatedWork W1491235841 @default.
W2286232018 hasRelatedWork W1964898256 @default.
W2286232018 hasRelatedWork W1970990212 @default.
W2286232018 hasRelatedWork W1981567206 @default.
W2286232018 hasRelatedWork W1981606991 @default.
W2286232018 hasRelatedWork W2032956181 @default.
W2286232018 hasRelatedWork W2049130216 @default.
W2286232018 hasRelatedWork W2069019880 @default.
W2286232018 hasRelatedWork W2079697748 @default.
W2286232018 hasRelatedWork W2081308460 @default.
W2286232018 hasRelatedWork W2090929360 @default.
W2286232018 hasRelatedWork W2102777859 @default.
W2286232018 hasRelatedWork W2175060787 @default.
W2286232018 hasRelatedWork W2338701266 @default.
W2286232018 hasRelatedWork W2470096999 @default.
W2286232018 hasRelatedWork W2492326185 @default.
W2286232018 hasRelatedWork W2537426197 @default.
W2286232018 hasRelatedWork W2626800051 @default.
W2286232018 hasRelatedWork W145074267 @default.
W2286232018 isParatext "false" @default.
W2286232018 isRetracted "false" @default.
W2286232018 magId "2286232018" @default.
W2286232018 workType "article" @default.