The deaminase APOBEC3B triggers the death of cells lacking uracil DNA glycosylase

Serebrenik, Artur A.; Starrett, Gabriel J.; Leenen, S; Jarvis, Matthew C.; Shaban, Nadine M.; Salamango, Daniel J.; Nilsen, Hilde; Brown, William L.; Harris, Reuben S.

doi:10.1073/pnas.1904024116

Cited by 35 publications

(58 citation statements)

References 49 publications

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“…Our findings establish UNG2 as a novel and ubiquitous target for HDACi-mediated degradation. This may expand indications for HDACi towards synthetic lethality in APOBEC3B expressing tumors [10] and to increase efficiency of deaminase-mediated CRISPR-Cas9 gene therapy [11]. Our results may also aid efforts to purge HIV viruses from latent reservoirs and treatment of autoimmune disease.…”

Section: Introductionmentioning

confidence: 75%

“…Finally, depletion of UNG was recently shown to induce synthetic lethality in APOBEC3B overexpressing cancers [10]. Many cancers overexpress APOBEC3B or harbor high kataegis mutational signatures conforming to deamination by the APOBEC/AID family of cytidine deaminases.…”

Section: Discussionmentioning

confidence: 99%

“…Lack of UNG mediates B-cell lymphoma in mice [33] and compromised immunoglobulin (Ig) CSR in humans due to impaired UNG2-mediated excision of uracils induced by activation induced deaminase (AID) at Ig switch regions [34]. UNG2 loss may also aggravate genomic instability in APOBEC3B expressing cancers [10]. Notably, three of the four proteins that helps activate the T-cell receptor (TCR) in the TCR complex CD3E (CD3ε), CD247 (CD3ζ) and CD3D (CD3δ) were among the ten most downregulated (1.9-fold) in Jurkat following SAHA treatment (Table 2), in agreement with earlier findings [35] and may explain the mono-therapy effects of HDACis in peripheral T-cell lymphomas such as CTCL, where T cell receptor activation can be a sustaining factor [36].…”

Section: Sudhl5 (Logmentioning

confidence: 99%

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HDACi mediate UNG2 depletion, dysregulated genomic uracil and altered expression of oncoproteins and tumor suppressors in B- and T-cell lines

et al. 2020

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Background: HDAC inhibitors (HDACi) belong to a new group of chemotherapeutics that are increasingly used in the treatment of lymphocyte-derived malignancies, but their mechanisms of action remain poorly understood. Here we aimed to identify novel protein targets of HDACi in Band T-lymphoma cell lines and to verify selected candidates across several mammalian cell lines. Methods: Jurkat T-and SUDHL5 B-lymphocytes were treated with the HDACi SAHA (vorinostat) prior to SILAC-based quantitative proteome analysis. Selected differentially expressed proteins were verified by targeted mass spectrometry, RT-PCR and western analysis in multiple mammalian cell lines. Genomic uracil was quantified by LC-MS/MS, cell cycle distribution analyzed by flow cytometry and class switch recombination monitored by FACS in murine CH12F3 cells. Results: SAHA treatment resulted in differential expression of 125 and 89 proteins in Jurkat and SUDHL5, respectively, of which 19 were commonly affected. Among these were several oncoproteins and tumor suppressors previously not reported to be affected by HDACi. Several key enzymes determining the cellular dUTP/dTTP ratio were downregulated and in both cell lines we found robust depletion of UNG2, the major glycosylase in genomic uracil sanitation. UNG2 depletion was accompanied by hyperacetylation and mediated by increased proteasomal degradation independent of cell cycle stage. UNG2 degradation appeared to be ubiquitous and was observed across several mammalian cell lines of different origin and with several HDACis. Loss of UNG2 was accompanied by 30-40% increase in genomic uracil in freely cycling HEK cells and reduced immunoglobulin class-switch recombination in murine CH12F3 cells. Conclusion: We describe several oncoproteins and tumor suppressors previously not reported to be affected by HDACi in previous transcriptome analyses, underscoring the importance of proteome analysis to identify cellular effectors of HDACi treatment. The apparently ubiquitous depletion of UNG2 and PCLAF establishes DNA base excision repair and translesion synthesis as novel pathways affected by HDACi treatment. Dysregulated genomic uracil

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Section: Introductionmentioning

confidence: 75%

Section: Discussionmentioning

confidence: 99%

Section: Sudhl5 (Logmentioning

confidence: 99%

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HDACi mediate UNG2 depletion, dysregulated genomic uracil and altered expression of oncoproteins and tumor suppressors in B- and T-cell lines

et al. 2020

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“…APOBEC3B is a cytosine deaminase that converts cytosine to uracil and causes an accumulation of C to T signature mutations in cancer genomes. A knockout of UNG has been demonstrated to kill APOBEC3B expressing cells due to an accumulation of uracil lesions in a mechanism dependent on non-canonical mismatch repair (MMR) [ 20 ]. Consequently, there is a need to develop specific small molecule inhibitors to UNG.…”

Section: Inhibitors To the Ber Enzymesmentioning

confidence: 99%

Base excision repair and its implications to cancer therapy

Grundy

Parsons

2020

Essays in Biochemistry

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Abstract Base excision repair (BER) has evolved to preserve the integrity of DNA following cellular oxidative stress and in response to exogenous insults. The pathway is a coordinated, sequential process involving 30 proteins or more in which single strand breaks are generated as intermediates during the repair process. While deficiencies in BER activity can lead to high mutation rates and tumorigenesis, cancer cells often rely on increased BER activity to tolerate oxidative stress. Targeting BER has been an attractive strategy to overwhelm cancer cells with DNA damage, improve the efficacy of radiotherapy and/or chemotherapy, or form part of a lethal combination with a cancer specific mutation/loss of function. We provide an update on the progress of inhibitors to enzymes involved in BER, and some of the challenges faced with targeting the BER pathway.

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“…Apolipoprotein B mRNA editing enzyme catalytic polypeptide-like 3B (APOBEC3B), an antiviral cytidine deaminase that induces DNA mutations, was considered as a medium for cancer development and therapeutic resistance [36]. Recent study have shown that the overexpression of APOBEC3B in tumor increased the resistance to chemotherapy and triggered anti-tumor T cells [37].…”

Section: Discussionmentioning

confidence: 99%

APOBEC3B and SPAG5, the Target Genes of miR-539, Involved into Imatinib-Resistant of Gastrointestinal Stromal Tumors

Zhang¹,

Liu²,

Li³

et al. 2020

Preprint

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Background: Although imatinib can effectively treat gastrointestinal stromal tumor (GIST), some patients are still resistant to it or cannot tolerate the adverse reactions of the drug. This study aimed to investigate potential miRNAs, mRNA and tumor-infiltrating lymphocytes (TILs) associated with the prognosis of imatinib-resistant GIST.Methods: mRNA, miRNA sequencing data and patient clinic traits of primary (imatinib-naive) and imatinib-resistant GIST were obtained from GEO (Gene Expression Omnibus) database. A systems biology approach combining Weighted co-expression network analysis (WGCNA) and differential expression analysis were utilized to detect the imatinib-resistant-related miRNA and gene modules and construct a miRNA-gene network. Tumor-infiltrating immune cells were analyzed by Estimating the Proportion of Immune and Cancer cells (EPIC) and Tumor-Immune System Interactions (TISIDB). miR-539 was measured by qRT-PCR. SPAG5 and APOBEC3B was measured by qRT-PCR and WB. Transforming growth factor (TGF)-β and interleukin (IL)-10 were assessed with enzyme-linked immunosorbent assay (ELISA). The proportions of CD4+ T cells, CD8+ T cells , NK cells and B cells in tumor-infiltrating lymphocyteswere analyzed via flow cytometry (FCM).Results: Two gene modules (brown and yellow) and one miRNA module were associated with the imatinib-resistant. Two hub genes (APOBEC3B and SPAG5) were associated with the imatinib-resistant. Three hub miRNAs were identified to be related to imatinib-resistant (miR-539, miR-376b and miR-18b). G1/S transition of mitotic cell cycle, G2/M transition of mitotic cell cycle, and cell proliferation were common pathways of the gene modules and miRNA module. apolipoprotein B mRNA editing catalytic polypeptide-like 3B (APOBEC3B) and Sperm-associated antigen 5 (SPAG5), which were both target genes of miR-539 was located at the core of miRNA–gene network. APOBEC3B (rho=0.509, p < 2.2e-16) and SPAG5 (rho=0.468, p < 2.2e-16) was positive correlated with the infiltration levels of activated CD4+ T cells. he proportions of CD4+ T cells, and the mRNA and protein relative expression of APOBEC3B and SPAG5 in imatinib-resistant tumor samples significantly increased as compared with tumor samples in imatinib-naive group. Imatinib-resistant tumor samples exhibited significantly downregulation of miR-539 and TGF-β1. Over-expression of miR-539 sensitized imatinib resistant GIST48 cells and increased the secretion of TGF-β1 by inhibiting APOBEC3B and SPAG5.Conclusion: APOBEC3B and SPAG5, the target genes of miR-539 may play as key factor for imatinib-resistant GIST by increasing the proportion of tumor-infiltrated activated CD4+ T cells via TGF-β1. These findings help to advance the understanding of imatinib-resistant GIST and provide potential therapeutic targets.

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The deaminase APOBEC3B triggers the death of cells lacking uracil DNA glycosylase

Cited by 35 publications

References 49 publications

HDACi mediate UNG2 depletion, dysregulated genomic uracil and altered expression of oncoproteins and tumor suppressors in B- and T-cell lines

HDACi mediate UNG2 depletion, dysregulated genomic uracil and altered expression of oncoproteins and tumor suppressors in B- and T-cell lines

Base excision repair and its implications to cancer therapy

APOBEC3B and SPAG5, the Target Genes of miR-539, Involved into Imatinib-Resistant of Gastrointestinal Stromal Tumors

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