Ordering of mutations in acute myeloid leukemia with partial tandem duplication of MLL (MLL-PTD)

Sun, Qi‐Yun; Ding, Ling-Wen; Tan, Kar Tong; Chien, Wenwen; Mayakonda, Anand; Lin, De; Loh, Xin Yi; Xiao, Jin; Meggendorfer, Manja; Alpermann, Tamara; Garg, Manoj; Lim, Su Lin; Madan, Vikas; Hattori, Norimichi; Nagata, Yasunobu; Miyano, Satoru; Yeoh, Allen Eng Juh; Hou, Hsin‐An; Jiang, Yan; Takao, Sumiko; Liu, L. Z.; Tan, Si Ying; Lill, Michael; Hayashi, Mutsumi; Kinoshita, Akitoshi; Kantarjian, Hagop M.; Kornblau, S.; Ogawa, Seishi; Haferlach, Torsten; Yang, Henry; Koeffler, H. Phillip

doi:10.1038/leu.2016.160

Cited by 71 publications

(89 citation statements)

References 41 publications

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“…Similar results were reported in a second publication [26], but this study also found that the combination of cohesin mutations with alterations in tyrosine kinases conferred a greater risk of relapse in patients with an otherwise “favorable” prognosis [26]. Lastly, recent studies have found that 26% of patients with MLL-PTD leukemia harbor cohesin mutations [27], but additional translocations have not been definitively studied thus far. Whether cohesin mutations cooperate or antagonize other common AML translocations remains unknown.…”

Section: Cohesin Mutations In Myeloid Neoplasmssupporting

confidence: 84%

Cohesin Mutations in Myeloid Malignancies

et al. 2017

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Acute Myeloid Leukemia (AML) is a hematologic malignancy with a poor prognosis. Recent genome-wide sequencing studies have identified frequent mutations in genes encoding members of the cohesin complex. Mutations in cohesin contribute to myeloid malignancies by conferring enhanced self-renewal of hematopoietic stem and progenitor cells but the mechanisms behind this phenotype have not been fully elucidated. Of note, cohesin mutations are highly prevalent in acute megakaryocytic leukemia associated with Down syndrome (DS-AMKL), where they occur in over half of patients. Evidence suggests that cohesin mutations alter gene expression through changes in chromatin accessibility and/or aberrant targeting of epigenetic complexes. In this review we discuss the pathogenic mechanisms by which cohesin mutations contribute to myeloid malignancies.

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Section: Cohesin Mutations In Myeloid Neoplasmssupporting

confidence: 84%

Cohesin Mutations in Myeloid Malignancies

et al. 2017

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“…Recently, several groups of researchers, including ourselves, uncovered the persistence of preleukemic clone at remission in adult AML, by showing the retention of canonical AML mutations with high VAF in remission samples (10,46-48). However, this scenario seems unlikely to be the case in pediatric ALL as our NGS data suggest that none of the somatic mutations persisted in matched remission samples (except for 2 cases with germline TP53 mutations and one case with a CREBBP stop-gain mutation that persisted in remission, which is likely also a germline mutation).…”

Section: Discussionmentioning

confidence: 99%

“…Illumina paired-end reads were aligned to NCBI build 37 using Novoalign, and somatic variants were called using Mutect (for single nucleotide variants, SNVs, LOD ≥ 6.3), VarScan (for SNVs and Indels, mutant supported by at least 6 reads, min-coverage ≥10, somatic-p-value ≤0.07, min-tumor-variant-freq ≥0.10, normal-variant-freq ≤0.05) and Pindel [for Indels, only indels that were less than 60bp long were retained (except for FLT3 , all the candidate mutations of FLT3 gene were retained for further analysis of potential internal tandem duplication (ITD) event), mutant supported by at least 6 reads and at least a 5% VAF]. For FLT3 -ITD detection, the Bam files were further analyzed using Pindel as described previously (10). All the candidate mutations were filtered with dbSNP131 [latest versions of the dbSNP database were not utilized as it contains some well characterized cancer mutations.…”

Section: Methodsmentioning

confidence: 99%

“…All the candidate mutations were filtered with dbSNP131 [latest versions of the dbSNP database were not utilized as it contains some well characterized cancer mutations. For example, KRAS G12D mutation was annotated as SNP rs121913529 in dbSNP137 and dbSNP138 (10)]; allele >0.1% in 1000 genome sequencing project or ESP5400 database and repetitive and low complexity regions (genomic SuperDups track, UCSC Genome Browser). Variants that appeared more than once in our in-house panel of normal controls database of 200+ samples were also removed.…”

Section: Methodsmentioning

confidence: 99%

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Mutational Landscape of Pediatric Acute Lymphoblastic Leukemia

et al. 2017

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Current standard of care for patients with pediatric acute lymphoblastic leukemia (ALL) is mainly effective, with high remission rates after treatment. However, the genetic perturbations that give rise to this disease remain largely undefined, limiting the ability to address resistant tumors or develop less toxic targeted therapies. Here we report the use of next generation sequencing to interrogate the genetic and pathogenic mechanisms of 240 pediatric ALL cases with their matched remission samples. Commonly mutated genes fell into several categories, including RAS/receptor tyrosine kinases, epigenetic regulators, transcription factors involved in lineage commitment and the p53/cell cycle pathway. Unique recurrent mutational hotspots were observed in epigenetic regulators CREBBP (R1446C/H), WHSC1 (E1099K) and the tyrosine kinase FLT3 (K663R, N676K). The mutant WHSC1 was established as a gain-of-function oncogene, while the epigenetic regulator ARID1A and transcription factor CTCF were functionally identified as potential tumor suppressors. Analysis of 28 diagnosis/relapse trio patients plus 10 relapse cases revealed four evolutionary paths and uncovered the ordering of acquisition of mutations in these patients. This study provides a detailed mutational portrait of pediatric ALL and gives insights into the molecular pathogenesis of this disease.

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“…It is currently under discussion whether cytoreduction upon HU therapy selects for TP53* mutated cells. A recent study analyzed the impact of TP53* in MPN patients and, although it is common that at least one somatic TP53* allele is transcribed in patient cells, the authors did not find a direct association between TP53 inactivation and HU resistance or blast transformation [33]. TP53 can also interact with STAT3 and STAT5 [39,40] and it induces mRNA expression of STAT5A , but not of STAT5B [41].…”

Section: Targets In Mpn and Driver Mutationsmentioning

confidence: 99%

Emerging therapeutic targets in myeloproliferative neoplasms and peripheral T-cell leukemia and lymphomas

Orlova

Wingelhofer

Neubauer

et al. 2017

Expert Opinion on Therapeutic Targets

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Introduction: Hematopoietic neoplasms are often driven by gain-of-function mutations of the JAK-STAT pathway together with mutations in chromatin remodeling and DNA damage control pathways. The interconnection between the JAK-STAT pathway, epigenetic regulation or DNA damage control is still poorly understood in cancer cell biology. Areas covered: Here, we focus on a broader description of mutational insights into myeloproliferative neoplasms and peripheral T-cell leukemia and lymphomas, since sequencing efforts have identified similar combinations of driver mutations in these diseases covering different lineages. We summarize how these pathways might be interconnected in normal or cancer cells, which have lost differentiation capacity and drive oncogene transcription. Expert opinion: Due to similarities in driver mutations including epigenetic enzymes, JAK-STAT pathway activation and mutated checkpoint control through TP53, we hypothesize that similar therapeutic approaches could be of benefit in these diseases. We give an overview of how driver mutations in these malignancies contribute to hematopoietic cancer initiation or progression, and how these pathways can be targeted with currently available tools.

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Ordering of mutations in acute myeloid leukemia with partial tandem duplication of MLL (MLL-PTD)

Cited by 71 publications

References 41 publications

Cohesin Mutations in Myeloid Malignancies

Cohesin Mutations in Myeloid Malignancies

Mutational Landscape of Pediatric Acute Lymphoblastic Leukemia

Emerging therapeutic targets in myeloproliferative neoplasms and peripheral T-cell leukemia and lymphomas

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