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Somatic variants in TET2 and DNMT3A are founding mutations in hematological malignancies that affect the epigenetic regulation of DNA methylation. Mutations in both genes often co-occur with activating mutations in genes encoding oncogenic tyrosine kinases such as FLT3 ITD , BCR-ABL1, JAK2 V617F , and MPL W515L , or with mutations affecting related signaling pathways such as NRAS G12D and CALR del52 . Here, we show that TET2 and DNMT3A mutations exert divergent roles in regulating DNA repair activities in leukemia cells expressing these oncogenes. Malignant TET2-deficient cells displayed downregulation of BRCA1 and LIG4, resulting in reduced activity of BRCA1/2-mediated homologous recombination (HR) and DNA-PK-mediated non-homologous end-joining (D-NHEJ), respectively. TET2-deficient cells relied on PARP1-mediated alternative NHEJ (Alt-NHEJ) for protection from the toxic effects of spontaneous and drug-induced DNA double-strand breaks. Conversely, DNMT3A-deficient cells favored HR/D-NHEJ owing to downregulation of PARP1 and reduction of Alt-NHEJ. Consequently, malignant TET2-deficient cells were sensitive to PARP inhibitor (PARPi) treatment in vitro and in vivo , whereas DNMT3A-deficient cells were resistant. Disruption of TET2 dioxygenase activity or TET2-Wilms' tumor 1 (WT1)-binding ability was responsible for DNA repair defects and sensitivity to PARPi associated with TET2 deficiency. Moreover, mutation or deletion of WT1 mimicked the effect of TET2 mutation on DSB repair activity and sensitivity to PARPi. Collectively, these findings reveal that TET2 and WT1 mutations may serve as biomarkers of synthetic lethality triggered by PARPi, which should be explored therapeutically. SIGNIFICANCE: TET2 and DNMT3A mutations affect distinct DNA repair mechanisms and govern the differential sensitivities of oncogenic tyrosine kinase-positive malignant hematopoietic cells to PARP inhibitors.

Titel:	TET2 and DNMT3A Mutations Exert Divergent Effects on DNA Repair and Sensitivity of Leukemia Cells to PARP Inhibitors.
Autor/in / Beteiligte Person:	Maifrede, S ; Le, BV ; Nieborowska-Skorska, M ; Golovine, K ; Sullivan-Reed, K ; Dunuwille, WMB ; Nacson, J ; Hulse, M ; Keith, K ; Madzo, J ; Caruso, LB ; Gazze, Z ; Lian, Z ; Padella, A ; Chitrala, KN ; Bartholdy, BA ; Matlawska-Wasowska, K ; Di Marcantonio, D ; Simonetti, G ; Greiner, G ; Sykes, SM ; Valent, P ; Paietta, EM ; Tallman, MS ; Fernandez, HF ; Litzow, MR ; Minden, MD ; Huang, J ; Martinelli, G ; Vassiliou, GS ; Tempera, I ; Piwocka, K ; Johnson, N ; Challen, GA ; Skorski, T
Link:	Full Text Finder (Volltext)
Zeitschrift:	Cancer research, Jg. 81 (2021-10-01), Heft 19, S. 5089-5101
Veröffentlichung:	Baltimore, Md. : American Association for Cancer Research ; <i>Original Publication</i>: Chicago [etc.], 2021
Medientyp:	academicJournal
ISSN:	1538-7445 (electronic)
DOI:	10.1158/0008-5472.CAN-20-3761
Schlagwort:	Animals CRISPR-Cas Systems Cell Line, Tumor Disease Models, Animal Dose-Response Relationship, Drug Gene Knockdown Techniques Genotype Humans Leukemia Mice Mice, Transgenic Models, Biological Neoplastic Stem Cells Xenograft Model Antitumor Assays DNA Methyltransferase 3A genetics DNA Repair DNA-Binding Proteins genetics Dioxygenases genetics Drug Resistance, Neoplasm genetics Mutation Poly(ADP-ribose) Polymerase Inhibitors pharmacology
Sonstiges:	Nachgewiesen in: MEDLINE Sprachen: English Publication Type: Journal Article; Research Support, N.I.H., Extramural; Research Support, Non-U.S. Gov't Language: English [Cancer Res] 2021 Oct 01; Vol. 81 (19), pp. 5089-5101. <i>Date of Electronic Publication: </i>2021 Jul 02. MeSH Terms: DNA Repair* ; Mutation* ; DNA Methyltransferase 3A / genetics ; DNA-Binding Proteins / genetics ; Dioxygenases / genetics ; Drug Resistance, Neoplasm / genetics ; Poly(ADP-ribose) Polymerase Inhibitors / *pharmacology ; Animals ; CRISPR-Cas Systems ; Cell Line, Tumor ; Disease Models, Animal ; Dose-Response Relationship, Drug ; Gene Knockdown Techniques ; Genotype ; Humans ; Leukemia ; Mice ; Mice, Transgenic ; Models, Biological ; Neoplastic Stem Cells ; Xenograft Model Antitumor Assays References: Mol Cell. 2015 Feb 19;57(4):662-673. (PMID: 25601757) ; Nat Rev Cancer. 2008 Dec;8(12):957-67. (PMID: 19005492) ; Clin Cancer Res. 2013 Sep 15;19(18):5003-15. 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(PMID: 12070033) Grant Information: UG1 CA233290 United States CA NCI NIH HHS; UG1 CA189859 United States CA NCI NIH HHS; R01 DK102428 United States DK NIDDK NIH HHS; UG1 CA232760 United States CA NCI NIH HHS; R01 GM124449 United States GM NIGMS NIH HHS; R01 HL147978 United States HL NHLBI NIH HHS; R01 CA227830 United States CA NCI NIH HHS; R01 CA244044 United States CA NCI NIH HHS; P30 CA010815 United States CA NCI NIH HHS; U24 CA196172 United States CA NCI NIH HHS; P30 CA008748 United States CA NCI NIH HHS; R01 CA214799 United States CA NCI NIH HHS; R01 GM135293 United States GM NIGMS NIH HHS; R01 CA247707 United States CA NCI NIH HHS; R01 CA186238 United States CA NCI NIH HHS; U10 CA180820 United States CA NCI NIH HHS; R01 CA237286 United States CA NCI NIH HHS; T32 CA009035 United States CA NCI NIH HHS Substance Nomenclature: 0 (DNA-Binding Proteins) ; 0 (DNMT3A protein, human) ; 0 (Poly(ADP-ribose) Polymerase Inhibitors) ; EC 1.13.11.- (Dioxygenases) ; EC 1.13.11.- (TET2 protein, human) ; EC 2.1.1.37 (DNA Methyltransferase 3A) Entry Date(s): Date Created: 20210703 Date Completed: 20220103 Latest Revision: 20240326 Update Code: 20240326 PubMed Central ID: PMC8487956

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TET2 and DNMT3A Mutations Exert Divergent Effects on DNA Repair and Sensitivity of Leukemia Cells to PARP Inhibitors.