Exome sequencing identifies somatic mutations of DNA methyltransferase gene DNMT3A in acute monocytic leukemia

Yan, Xiaojing; Xu, Jie; Gu, Zhaohui; Pan, Chun-Ming; Lu, Gang; Shen, Yang; Shi, Jingyi; Zhu, Yong‐Mei; Tang, Lin; Zhang, Xiaowei; Liang, Wenxue; Mi, Jian-Qing; Song, Huai-Dong; Li, Keqin; Chen, Zhu; Chen, Sai‐Juan

doi:10.1038/ng.788

Cited by 719 publications

(702 citation statements)

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“…We and others 24,25,29 --31,44 found that DNMT3A mutations were strongly associated with FAB M4/M5 subtypes, and often co-occurred with NPM1 or IDH1 mutations in AML patients, suggesting that the oncogenic actions of these mutations are not redundant. DNMT3A mutations were reported to be associated with older age, 24,25,30,31 but this feature was not observed in our cohort of adult CN-AML. Nevertheless, a link between age and the incidence of DNMT3A mutations is likely as these mutations seem to be extremely rare (o1%) in pediatric AML.…”

Section: Discussioncontrasting

confidence: 77%

“…45 --47 Among the 11 different DNMT3A mutations identified in our cohort, those affecting R882 residue were the most common, in agreement with previous reports. 24,25,29 Interestingly, the somatic R882 mutations in DNMT3A found in AML are analogous to the inherited R823G mutation in DNMT3B, which was discovered in a human syndrome characterized by immunodeficiency, centrosome instability and facial abnormalities (ICF) in association with defects in genomic methylation. 48,49 In AML, the exact pathogenic mechanism by which DNMT3A mutations act is still enigmatic.…”

Section: Discussionmentioning

confidence: 99%

“…However, the leukemogenic potential of DNMT3A mutations remains to be proven at an organism level. 25 Most DNMT3A mutants showed reduced enzymatic activity or aberrant affinity to histone H3 in vitro. 25,26 Using methyl-DNA immunoprecipitation chip analysis in AML samples with DNMT3A R882 mutations, Ley et al 24 identified 182 genomic regions with decreases in DNA methylation, while Yan et al 25 found almost 4000.…”

Section: Discussionmentioning

confidence: 99%

“…25 Most DNMT3A mutants showed reduced enzymatic activity or aberrant affinity to histone H3 in vitro. 25,26 Using methyl-DNA immunoprecipitation chip analysis in AML samples with DNMT3A R882 mutations, Ley et al 24 identified 182 genomic regions with decreases in DNA methylation, while Yan et al 25 found almost 4000. Anyway, DNMT3A mutations did not yield a specific pattern of altered DNA methylation, unlike other recurrent genetic abnormalities in AML, such as PML-RARA, CBFB-MYH11 or double CEBPA mutations.…”

Section: Discussionmentioning

confidence: 99%

“…50 Likewise, the influence of DNMT3A mutational status on gene expression profiles is yet unclear, and DNMT3A mutant AML was not found to have a common gene expression signature. 24,25 Further experiments are needed to identify genes whose expression is modulated by DNMT3A mutations and determine the biological effects of these mutations. We showed that DNMT3A mutations confer a poor prognosis in CN-AML, in line with previous studies in AML.…”

Section: Discussionmentioning

confidence: 99%

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Prognostic significance of DNA methyltransferase 3A mutations in cytogenetically normal acute myeloid leukemia: a study by the Acute Leukemia French Association

et al. 2012

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Recently, DNA methyltransferase 3A (DNMT3A) mutations have been identified in acute myeloid leukemia (AML), the highest frequency being found within cytogenetically normal (CN) AML. In this study, diagnostic samples from 123 adults younger than 60 years with primary CN-AML homogeneously treated in the Acute Leukemia French Association-9801 and -9802 trials were screened for mutations in DNMT3A-conserved domains by direct sequencing. Patients were also assessed for the presence of FLT3 (fms-like tyrosine kinase receptor-3), NPM1 (nucleophosmin), CEBPA, WT1 (Wilms tumor 1), IDH1 (isocitrate dehydrogenase 1) and IDH2 mutations. Thirty-eight mutations were detected in 36 patients (29%): 36 nucleotide substitutions, mostly affecting amino-acid residue R882 and two frameshift deletions. DNMT3A mutations were significantly associated with the French --American --British subtypes M4/M5 and the presence of NPM1 mutations. In the whole cohort, DNMT3A mutated patients had a shorter event-free survival (5-year EFS: 13% vs 32%, P ¼ 0.02) and overall survival (5-year OS: 23% vs 45%, P ¼ 0.02) compared with DNMT3A wild-type patients. In multivariate analysis including age, white blood cell count, NPM1/FLT3-internal tandem duplication/CEBPA risk group and DNMT3A mutational status, the presence of a DNMT3A mutation remained an independent adverse prognostic factor for EFS and OS, suggesting that testing for DNMT3A mutations could help further improve risk stratification in CN-AML.

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Section: Discussioncontrasting

confidence: 77%

Section: Discussionmentioning

confidence: 99%

Section: Discussionmentioning

confidence: 99%

Section: Discussionmentioning

confidence: 99%

Section: Discussionmentioning

confidence: 99%

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Prognostic significance of DNA methyltransferase 3A mutations in cytogenetically normal acute myeloid leukemia: a study by the Acute Leukemia French Association

et al. 2012

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The DNA methylation landscape of hematological malignancies: an update

2020

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The rapid advances in high‐throughput sequencing technologies have made it more evident that epigenetic modifications orchestrate a plethora of complex biological processes. During the last decade, we have gained significant knowledge about a wide range of epigenetic changes that crucially contribute to some of the most aggressive forms of leukemia, lymphoma, and myelodysplastic syndromes. DNA methylation is a key epigenetic player in the abnormal initiation, development, and progression of these malignancies, often acting in synergy with other epigenetic alterations. It also contributes to the acquisition of drug resistance. In this review, we summarize the role of DNA methylation in hematological malignancies described in the current literature. We discuss in detail the dual role of DNA methylation in normal and aberrant hematopoiesis, as well as the involvement of this type of epigenetic change in other aspects of the disease. Finally, we present a comprehensive overview of the main clinical implications, including a discussion of the therapeutic strategies that regulate or reverse aberrant DNA methylation patterns in hematological malignancies, including their combination with (chemo)immunotherapy.

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Characterising Somatic Mutations in Cancer Genome by Means of Next‐generation Sequencing

Chong

et al. 2012

Encyclopedia of Life Sciences

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Cancer genome sequencing studies have identified tens of thousands of somatic mutations in various human cancers to date. This data has started to generate new insights into mutation patterns and their differences between various cancers. Further, the mutation patterns have also helped to elucidate mechanism involved in generating mutations in cancer genome such as deoxyribonucleic acid (DNA) ‐repair processes and mutagen exposures. With the introduction of next‐generation sequencing technologies, cancer genome sequencing has evolved from a targeted sequencing approach to whole‐exome sequencing and whole‐genome sequencing (WGS) approaches. However, each sequencing approach has its strengths and limitations. It is widely anticipated that WGS would eventually replace targeted and exome sequencing. WGS offers a unique advantage to study structural variants or rearrangements and fusion genes in a single experiment, in addition to point mutations. However, currently the WGS is still prohibitively expensive for a large number of samples. Despite these technological advances, several challenges still remain, such as discerning driver mutations from benign mutations and collection of high‐quality primary tumour tissues to minimise tissue heterogeneity. Ultimately, a comprehensive delineation of the somatic mutations in the cancer genome would require WGS of a large number of samples from various cancer types and subtypes. Congruent to this goal, the International Cancer Genome Consortium was initiated and upon completion of the project, its data is expected to further enhance our knowledge and understanding of the biological mechanisms underlying cancer development. Key Concepts: Several sequencing approaches are available to decipher the somatic mutation profile of cancer genome, including targeted sequencing, whole‐exome sequencing (WES) and whole‐genome sequencing (WGS). Targeted sequencing is a hypothesis‐driven approach where candidate genes were often selected based on knowledge of previously reported mutated genes or their related functions in cancer development, such as the kinome or phosphatome. The ability to study different cancers and their subtypes in a comparatively higher throughput to exome and WGS is an important advantage of the targeted sequencing approach. The introduction of multiple commercial exome enrichment kits has circumvented the technical challenges in isolating the entire exome for sequencing. Although WES interrogates only approximately 1–2% of the entire human genome, the several hundred somatic mutations identified in WES studies have already prohibited all of them to be examined by follow‐up studies in larger sample series. The advances of NGS technologies and rapidly declining sequencing cost have enabled the completion of a number of WGS studies for various cancers. The patterns of somatic mutations provided by WGS are useful in elucidating the mechanisms of generating the mutations in cancer genome such as DNA‐repair processes and differences in mutagen exposure. A further advantage over the other two sequencing approaches of WGS is its ability to identify structural rearrangements. Although WES and WGS approaches have now been shown to be technically feasible, several challenges still remain. Delineating patterns of somatic mutations in the cancer genome require a comprehensive interrogation of cancer genomes (entire genome, exome or a large number of candidate genes) in series of up to hundreds of samples.

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Exome sequencing identifies somatic mutations of DNA methyltransferase gene DNMT3A in acute monocytic leukemia

Cited by 719 publications

References 46 publications

Prognostic significance of DNA methyltransferase 3A mutations in cytogenetically normal acute myeloid leukemia: a study by the Acute Leukemia French Association

Prognostic significance of DNA methyltransferase 3A mutations in cytogenetically normal acute myeloid leukemia: a study by the Acute Leukemia French Association

The DNA methylation landscape of hematological malignancies: an update

Characterising Somatic Mutations in Cancer Genome by Means of Next‐generation Sequencing

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