Author Correction: RNA cytosine methylation and methyltransferases mediate chromatin organization and 5-azacytidine response and resistance in leukaemia

Cheng, Jian; Chen, Li; Li, Yuan; Cloe, Adam; Ming, Yue; Wei, Jiangbo; Watanabe, Kenneth A.; Shammo, Jamile M.; Anastasi, John; Shen, Qi; Larson, Richard A.; He, Chuan; Beau, Michelle M. Le; Vardiman, James W.

doi:10.1038/s41467-018-04518-9

Cited by 11 publications

(9 citation statements)

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“…Given that alterations involving increased expression of NSUN2 are common in breast cancer [ 93 , 95 , 98 ], colon cancer [ 92 , 93 ], and lung cancer as suggested in the suggestions above, molecularly targeting this RNMT would appear to an attractive approach moving forward. While studies on NSUN2 have used azacytidine in the past [ 24 , 110 ], due to the previously poor responses to this drug observed in the past, newer approaches may be necessary to elicit effective responses in patients. For example, it may be possible to use agents targeting NSUN2 to increase the number of patients that may be suitable for checkpoint inhibitors.…”

Section: Discussionmentioning

confidence: 99%

“…Loss of the region containing NSUN3 has been reported as a common loss in lung adenocarcinomas of never-smokers at a frequency of 15% [ 109 ], and interestingly, this was the only coding gene in the region lost [ 109 ]. Mutation of NSUN3 has been shown to result in reduced mitochondrial protein translation and respiration [ 2 ], while some evidence has shown a role for NSUN3 in nuclear transcriptional regulation in leukemic cells [ 110 ].…”

Section: Known Roles For Nsun2 In Cancermentioning

confidence: 99%

“…Molecularly targeting m5C RNMTs using drugs previously developed to target DNMTs is a potential possibility as demonstrated from using Aza-IP [ 24 ] and preliminary in vitro data in leukemic cells, where novel RNA:m5C/RCMT-mediated chromatin structures form that modulate 5-AZA response/resistance [ 110 ]. Alternatively, it may be possible to target NSUN2-mediated events such as that shown for the lncRNA NMR in esophageal cancer, whereby NSUN2-methylated NMR interacts with the chromatin remodeling factor Bromodomain PHD Finger Transcription Factor (BPTF) [ 35 , 118 ] to regulate resistance to cisplatin.…”

Section: Known Roles For Nsun2 In Cancermentioning

confidence: 99%

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The RNA Methyltransferase NSUN2 and Its Potential Roles in Cancer

Chellamuthu

Gray

2020

Cells

115

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5-methylcytosine is often associated as an epigenetic modifier in DNA. However, it is also found increasingly in a plethora of RNA species, predominantly transfer RNAs, but increasingly found in cytoplasmic and mitochondrial ribosomal RNAs, enhancer RNAs, and a number of long noncoding RNAs. Moreover, this modification can also be found in messenger RNAs and has led to an increasing appreciation that RNA methylation can functionally regulate gene expression and cellular activities. In mammalian cells, the addition of m5C to RNA cytosines is carried out by enzymes of the NOL1/NOP2/SUN domain (NSUN) family as well as the DNA methyltransferase homologue DNMT2. In this regard, NSUN2 is a critical RNA methyltransferase for adding m5C to mRNA. In this review, using non-small cell lung cancer and other cancers as primary examples, we discuss the recent developments in the known functions of this RNA methyltransferase and its potential critical role in cancer.

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Section: Discussionmentioning

confidence: 99%

Section: Known Roles For Nsun2 In Cancermentioning

confidence: 99%

Section: Known Roles For Nsun2 In Cancermentioning

confidence: 99%

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The RNA Methyltransferase NSUN2 and Its Potential Roles in Cancer

Chellamuthu

Gray

2020

Cells

115

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“…In addition to its effect on DNA, azacitadine has been reported to inhibit the RNA methyltransferase, DNMT2 (96) suggesting that it's mechanism of action in myeloid neoplasms may be linked to modification of RNA. Consistent with this possibility, in a recent report, distinct RNA 5-methylcytosine methyltransferase chromatin complexes were demonstrated to mediate sensitivity vs. resistance to azacitadine (97). Up-regulation of antigen presentation pathways, such as MHC expression, are part of the mechanism by which HMA are described to recalibrate the immune micoenvironment promoting anti-tumor responses (98–103).…”

Section: Immunomodulation and Anti-leukemia Therapymentioning

confidence: 53%

The Interplay Between the Genetic and Immune Landscapes of AML: Mechanisms and Implications for Risk Stratification and Therapy

2019

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AML holds a unique place in the history of immunotherapy by virtue of being among the first malignancies in which durable remissions were achieved with “adoptive immunotherapy,” now known as allogeneic stem cell transplantation. The successful deployment of unselected adoptive cell therapy established AML as a disease responsive to immunomodulation. Classification systems for AML have been refined and expanded over the years in an effort to capture the variability of this heterogeneous disease and risk-stratify patients. Current systems increasingly incorporate information about cytogenetic alterations and genetic mutations. The advent of next generation sequencing technology has enabled the comprehensive identification of recurrent genetic mutations, many with predictive power. Recurrent genetic mutations found in AML have been intensely studied from a cell intrinsic perspective leading to the genesis of multiple, recently approved targeted therapies including IDH1/2-mutant inhibitors and FLT3-ITD/-TKD inhibitors. However, there is a paucity of data on the effects of these targeted agents on the leukemia microenvironment, including the immune system. Recently, the phenomenal success of checkpoint inhibitors and CAR-T cells has re-ignited interest in understanding the mechanisms leading to immune dysregulation and suppression in leukemia, with the objective of harnessing the power of the immune system via novel immunotherapeutics. A paradigm has emerged that places crosstalk with the immune system at the crux of any effective therapy. Ongoing research will reveal how AML genetics inform the composition of the immune microenvironment paving the way for personalized immunotherapy.

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“…The cause of NSUN2 up-regulation in solid tumours such as colorectal and oral cancers can be increased copy number (Okamoto et al, 2012). There is already emerging evidence for an impact of RNA m 5 C on drug sensitivity (Cheng et al, 2018), suggesting that this may be a fruitful avenue of research in the near future.…”

Section: Cancermentioning

confidence: 99%

Environmental epitranscriptomics

Çayır

Byun

Barrow

2020

Environmental Research

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This is a PDF file of an article that has undergone enhancements after acceptance, such as the addition of a cover page and metadata, and formatting for readability, but it is not yet the definitive version of record. This version will undergo additional copyediting, typesetting and review before it is published in its final form, but we are providing this version to give early visibility of the article. Please note that, during the production process, errors may be discovered which could affect the content, and all legal disclaimers that apply to the journal pertain.

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Author Correction: RNA cytosine methylation and methyltransferases mediate chromatin organization and 5-azacytidine response and resistance in leukaemia

Abstract: In the originally published version of this Article, the GAPDH loading control blot in Fig. 1a was inadvertently replaced with a duplicate of the DNMT2 blot in the same panel during assembly of the figure. This has now been corrected in both the PDF and HTML versions of the Article.

Cited by 11 publications

References 0 publications

The RNA Methyltransferase NSUN2 and Its Potential Roles in Cancer

The RNA Methyltransferase NSUN2 and Its Potential Roles in Cancer

The Interplay Between the Genetic and Immune Landscapes of AML: Mechanisms and Implications for Risk Stratification and Therapy

Environmental epitranscriptomics

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