FRINK Linked Data Fragments server

Matches in SemOpenAlex for { <https://semopenalex.org/work/W4200467940> ?p ?o ?g. }

• W4200467940 endingPage "900" @default.
• W4200467940 startingPage "888" @default.
• W4200467940 abstract "ATRX inactivation occurs with IDH1R132H and p53 mutations in over 80% of Grades II/III astrocytomas. It is believed that ATRX loss contributes to oncogenesis by dysregulating epigenetic and telomere mechanisms but effects on anti-glioma immunity have not been explored. This paper examines how ATRX loss contributes to the malignant and immunosuppressive phenotypes of IDH1R132H/p53mut glioma cells and xenografts.Isogenic astrocytoma cells (+/-IDH1R132H/+/-ATRXloss) were established in p53mut astrocytoma cell lines using lentivirus encoding doxycycline-inducible IDH1R132H, ATRX shRNA, or Lenti-CRISPR/Cas9 ATRX. Effects of IDH1R132H+/-ATRXloss on cell migration, growth, DNA repair, and tumorigenicity were evaluated by clonal growth, transwell and scratch assays, MTT, immunofluorence and immunoblotting assays, and xenograft growth. Effects on the expression and function of modulators of the immune microenvironment were quantified by qRT-PCR, immunoblot, T-cell function, macrophage polarization, and flow cytometry assays. Pharmacologic inhibitors were used to examine epigenetic drivers of the immunosuppressive transcriptome of IDH1R132H/p53mut/ATRXloss cells.Adding ATRX loss to the IDH1R132H/p53mut background promoted astrocytoma cell aggressiveness, induced expression of BET proteins BRD3/4 and an immune-suppressive transcriptome consisting of up-regulated immune checkpoints (e.g., PD-L1, PD-L2) and altered cytokine/chemokine profiles (e.g., IL33, CXCL8, CSF2, IL6, CXCL9). ATRX loss enhanced the capacity of IDH1R132H/p53mut cells to induce T-cell apoptosis, tumorigenic/anti-inflammatory macrophage polarization and Treg infiltration. The transcriptional and biological immune-suppressive responses to ATRX loss were enhanced by temozolomide and radiation and abrogated by pharmacologic BET inhibition.ATRX loss activates a BRD-dependent immune-suppressive transcriptome and immune escape mechanism in IDH1R132H/p53mut astrocytoma cells." @default.
• W4200467940 created "2021-12-31" @default.
• W4200467940 creator A5011340023 @default.
• W4200467940 creator A5014614164 @default.
• W4200467940 creator A5022191333 @default.
• W4200467940 creator A5027043430 @default.
• W4200467940 creator A5028344363 @default.
• W4200467940 creator A5030120953 @default.
• W4200467940 creator A5035964041 @default.
• W4200467940 creator A5043394718 @default.
• W4200467940 creator A5056581388 @default.
• W4200467940 creator A5061207404 @default.
• W4200467940 creator A5068043303 @default.
• W4200467940 creator A5080005941 @default.
• W4200467940 creator A5080576304 @default.
• W4200467940 creator A5090338647 @default.
• W4200467940 date "2021-12-24" @default.
• W4200467940 modified "2023-10-18" @default.
• W4200467940 title "ATRX loss promotes immunosuppressive mechanisms in IDH1 mutant glioma" @default.
• W4200467940 cites W1480357432 @default.
• W4200467940 cites W1501247525 @default.
• W4200467940 cites W1812256879 @default.
• W4200467940 cites W1986009297 @default.
• W4200467940 cites W2010573862 @default.
• W4200467940 cites W2013090484 @default.
• W4200467940 cites W2037466043 @default.
• W4200467940 cites W2057423047 @default.
• W4200467940 cites W2058947771 @default.
• W4200467940 cites W2066640259 @default.
• W4200467940 cites W2111424734 @default.
• W4200467940 cites W2115276344 @default.
• W4200467940 cites W2142630775 @default.
• W4200467940 cites W2149360266 @default.
• W4200467940 cites W2220215167 @default.
• W4200467940 cites W2292914130 @default.
• W4200467940 cites W2319404678 @default.
• W4200467940 cites W2404404965 @default.
• W4200467940 cites W2583978691 @default.
• W4200467940 cites W2588505042 @default.
• W4200467940 cites W2596261790 @default.
• W4200467940 cites W2611222875 @default.
• W4200467940 cites W2612431515 @default.
• W4200467940 cites W2617691667 @default.
• W4200467940 cites W2619583962 @default.
• W4200467940 cites W2765199703 @default.
• W4200467940 cites W2766773147 @default.
• W4200467940 cites W2768434280 @default.
• W4200467940 cites W2790178097 @default.
• W4200467940 cites W2792875887 @default.
• W4200467940 cites W2792919791 @default.
• W4200467940 cites W2794763378 @default.
• W4200467940 cites W2800556562 @default.
• W4200467940 cites W2807073094 @default.
• W4200467940 cites W2878436114 @default.
• W4200467940 cites W2883634139 @default.
• W4200467940 cites W2887976258 @default.
• W4200467940 cites W2896254157 @default.
• W4200467940 cites W2911943691 @default.
• W4200467940 cites W2916635720 @default.
• W4200467940 cites W2947216697 @default.
• W4200467940 cites W2950531883 @default.
• W4200467940 doi "https://doi.org/10.1093/neuonc/noab292" @default.
• W4200467940 hasPubMedId "https://pubmed.ncbi.nlm.nih.gov/34951647" @default.
• W4200467940 hasPublicationYear "2021" @default.
• W4200467940 type Work @default.
• W4200467940 citedByCount "18" @default.
• W4200467940 countsByYear W42004679402022 @default.
• W4200467940 countsByYear W42004679402023 @default.
• W4200467940 crossrefType "journal-article" @default.
• W4200467940 hasAuthorship W4200467940A5011340023 @default.
• W4200467940 hasAuthorship W4200467940A5014614164 @default.
• W4200467940 hasAuthorship W4200467940A5022191333 @default.
• W4200467940 hasAuthorship W4200467940A5027043430 @default.
• W4200467940 hasAuthorship W4200467940A5028344363 @default.
• W4200467940 hasAuthorship W4200467940A5030120953 @default.
• W4200467940 hasAuthorship W4200467940A5035964041 @default.
• W4200467940 hasAuthorship W4200467940A5043394718 @default.
• W4200467940 hasAuthorship W4200467940A5056581388 @default.
• W4200467940 hasAuthorship W4200467940A5061207404 @default.
• W4200467940 hasAuthorship W4200467940A5068043303 @default.
• W4200467940 hasAuthorship W4200467940A5080005941 @default.
• W4200467940 hasAuthorship W4200467940A5080576304 @default.
• W4200467940 hasAuthorship W4200467940A5090338647 @default.
• W4200467940 hasBestOaLocation W42004679401 @default.
• W4200467940 hasConcept C104317684 @default.
• W4200467940 hasConcept C121608353 @default.
• W4200467940 hasConcept C13373296 @default.
• W4200467940 hasConcept C177336024 @default.
• W4200467940 hasConcept C203014093 @default.
• W4200467940 hasConcept C2776689207 @default.
• W4200467940 hasConcept C2778227246 @default.
• W4200467940 hasConcept C501734568 @default.
• W4200467940 hasConcept C502942594 @default.
• W4200467940 hasConcept C54355233 @default.
• W4200467940 hasConcept C552990157 @default.
• W4200467940 hasConcept C555283112 @default.
• W4200467940 hasConcept C86803240 @default.
• W4200467940 hasConcept C8891405 @default.

• next