Landscape of genetic lesions in 944 patients with myelodysplastic syndromes

Haferlach, Torsten; Nagata, Yasunobu; Grossmann, Vera; Okuno, Yusuke; Bacher, Ulrike; Nagae, Genta; Schnittger, Susanne; Sanada, Masashi; Kon, Ayana; Alpermann, Tamara; Yoshida, Kenichi; Roller, Andreas; Nadarajah, Niroshan; Shiraishi, Yuichi; Shiozawa, Yusuke; Chiba, Kenichi; Tanaka, Hiroko; Koeffler, H. Phillip; Klein, Hans-Ulrich; Dugas, Martin; Aburatani, Hiroyuki; Kohlmann, Alexander; Miyano, Satoru; Haferlach, Claudia; Kern, Wolfgang; Ogawa, Seishi

doi:10.1038/leu.2013.336

Cited by 1,352 publications

(1,643 citation statements)

References 31 publications

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“…As previously reported we detected an increased number of genetic lesions in high‐risk WHO subtypes (Supporting Information Figure S3A) and found a correlation between the average number of genetic aberrations and the IPSS‐R prognostic risk score (Supporting Information Figure S3B) 1, 2. Interestingly, low risk patients displayed an increased number of somatic mutations compared to the number of lesions detected by CBA or SNP‐A.…”

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confidence: 83%

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Targeted deep sequencing of CD34+ cells from peripheral blood can reproduce bone marrow molecular profile in myelodysplastic syndromes

et al. 2018

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confidence: 83%

“…To identify molecular markers of clinical relevance, we screened genes previously reported to be frequently mutated in MDS and other myeloid malignancies 1, 2. The somatic origin of the variants was validated by comparison of the concurrent samples (BMC, PB‐CD34, and PB‐MC) with a paired germline sample, peripheral CD3 + cells (PB‐CD3).…”

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confidence: 99%

Targeted deep sequencing of CD34+ cells from peripheral blood can reproduce bone marrow molecular profile in myelodysplastic syndromes

et al. 2018

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“…Other MDS/AML-related genes were also recurrently mutated but at lower frequencies ( Figure 3). 18,20,66 The highly recurrent nature of well-characterized driver mutations indicates that they were selected by a Darwinian mechanism, rather than stochastically achieving a clonal dominance merely by a rapid expansion from a small number of residual stem cells ("bottleneck"). 9 In several patients, some of these genes, including PIGA, DNMT3A, ASXL1, BOCR, and RUNX1, harbor multiple, independent mutations, suggesting a strong selective pressure favoring evolution of cells having these mutations ( Figure 3A).…”

Section: Characteristics Of Mutations In Aamentioning

confidence: 99%

Clonal hematopoiesis in acquired aplastic anemia

Ogawa

2016

Blood

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Clonal hematopoiesis (CH) in aplastic anemia (AA) has been closely linked to the evolution of late clonal disorders, including paroxysmal nocturnal hemoglobinuria and myelodysplastic syndromes (MDS)/acute myeloid leukemia (AML), which are common complications after successful immunosuppressive therapy (IST). With the advent of high-throughput sequencing of recent years, the molecular aspect of CH in AA has been clarified by comprehensive detection of somatic mutations that drive clonal evolution. Genetic abnormalities are found in ∼50% of patients with AA and, except for PIGA mutations and copy-neutral loss-of-heterozygosity, or uniparental disomy (UPD) in 6p (6pUPD), are most frequently represented by mutations involving genes commonly mutated in myeloid malignancies, including DNMT3A, ASXL1, and BCOR/BCORL1. Mutations exhibit distinct chronological profiles and clinical impacts. BCOR/BCORL1 and PIGA mutations tend to disappear or show stable clone size and predict a better response to IST and a significantly better clinical outcome compared with mutations in DNMT3A, ASXL1, and other genes, which are likely to increase their clone size, are associated with a faster progression to MDS/AML, and predict an unfavorable survival. High frequency of 6pUPD and overrepresentation of PIGA and BCOR/BCORL1 mutations are unique to AA, suggesting the role of autoimmunity in clonal selection. By contrast, DNMT3A and ASXL1 mutations, also commonly seen in CH in the general population, indicate a close link to CH in the aged bone marrow, in terms of the mechanism for selection. Detection and close monitoring of somatic mutations/evolution may help with prediction and diagnosis of clonal evolution of MDS/AML and better management of patients with AA.

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“…Previous studies on MDS patients showed that mutations in ASXL1, ETV6, EZH2, IDH2, RUNX1, and TP53 are predictors of poor overall survival in MDS patients independently of other established risk factors. [11][12][13] Furthermore the splicing machinery is one of the most frequently affected pathways in MDS, 14 and mutations in SRSF2 have been shown to be independently associated with a negative prognosis for overall survival and AML transformation. 15 Recently, several of these gene mutations were identified as specific for s-AML in comparison to de novo AML underlining their function in dysplastic differentiation since they occur already at the stage of MDS.…”

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confidence: 99%