High incidence of somatic mutations in the AML1/RUNX1 gene in myelodysplastic syndrome and low blast percentage myeloid leukemia with myelodysplasia

Harada, Hironori; Harada, Yuka; Niimi, Hiromasa; Kyo, Taiichi; Kimura, Akiro; Inaba, Toshiya

doi:10.1182/blood-2003-09-3074

Cited by 256 publications

(265 citation statements)

References 31 publications

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“…19 We found BM mononuclear cells from MDS/AML patients harboring RUNX1-C-terminal mutations had significantly lower GAD-D45A expression compared with those from MDS/AML patients with WT RUNX1 (P ¼ 0.0233; Figure 6). …”

Section: Runx1 Transcriptionally Regulates Gadd45a Expressionmentioning

confidence: 92%

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C-terminal mutation of RUNX1 attenuates the DNA-damage repair response in hematopoietic stem cells

et al. 2011

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Loss-of-function mutations of RUNX1 have been found in acute myeloid leukemia (AML) and myelodysplastic syndromes (MDSs). Although several reports have suggested roles for RUNX1 as a tumor suppressor, its precise function remains unknown. Because gene alterations of RUNX1 by themselves do not lead to the development of leukemia in mouse models, additional mutation(s) would be required for leukemia development. Here, we report that the C-terminal deletion mutant of RUNX1, RUNX1dC, attenuates DNA-damage repair responses in hematopoietic stem/progenitor cells. cH2AX foci, which indicate the presence of DNA double-strand breaks, were more abundantly accumulated in RUNX1dC-transduced lineage À Sca1 þ c-kit þ (LSK) cells than in mock-transduced LSK cells both in a steady state and after c-ray treatment. Expression profiling by real-time -PCR array revealed RUNX1dC represses the expression of Gadd45a, a sensor of DNA stress. Furthermore, bone marrow cells from MDS/AML patients harboring the RUNX1-C-terminal mutation showed significantly lower levels of GADD45A expression compared with those from MDS/AML patients with wild-type RUNX1. As for this mechanism, we found that RUNX1 directly regulates the transcription of GADD45A and that RUNX1 and p53 synergistically activate the GADD45A transcription. Together, these results suggest Gadd45a dysfunction due to RUNX1 mutations can cause additional mutation(s) required for multi-step leukemogenesis.

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Section: Runx1 Transcriptionally Regulates Gadd45a Expressionmentioning

confidence: 92%

“…19,38,39 We speculate that a RUNX1 mutation may be a cause of additional mutation(s) through the impaired DDR response. In future studies, whole genome analysis of MDS/AML samples harboring RUNX1 mutations would clarify the role of RUNX1 mutations in the occurrence of genetic abnormalities in these patients.…”

Section: Discussionmentioning

confidence: 99%

C-terminal mutation of RUNX1 attenuates the DNA-damage repair response in hematopoietic stem cells

et al. 2011

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“…C-terminal mutations are seen at lower frequency and almost exclusively in MDS or AML following MDS, and seem to be associated with poor prognosis. 132 A high frequency (40%) of N-terminal AML1 mutation has also been observed in t-AML and t-MDS. 132 Some monoallelic mutations may act in a dominant-negative manner through inhibition of the effects the remaining WT AML1.…”

Section: Aml1mentioning

confidence: 99%

“…132 A high frequency (40%) of N-terminal AML1 mutation has also been observed in t-AML and t-MDS. 132 Some monoallelic mutations may act in a dominant-negative manner through inhibition of the effects the remaining WT AML1. This hypothesis was confirmed by Osato et al and Imai et al, 124,126 who demonstrated that some AML1 gene missense mutation cotransfected with WT AML1 abolished transactivation of the M-CSF receptor promoter.…”

Section: Aml1mentioning

confidence: 99%

Cooperating gene mutations in acute myeloid leukemia: a review of the literature

et al. 2008

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Acute myeloid leukemia (AML) is a heterogeneous group of neoplastic disorders with great variability in clinical course and response to therapy, as well as in the genetic and molecular basis of the pathology. Major advances in the understanding of leukemogenesis have been made by the characterization and the study of acquired cytogenetic abnormalities, particularly reciprocal translocations observed in AML. Besides these major cytogenetic abnormalities, gene mutations also constitute key events in AML pathogenesis. In this review, we describe the contribution of known gene mutations to the understanding of AML pathogenesis and their clinical significance. To gain more insight in this understanding, we clustered these alterations in three groups: (1) mutations affecting genes that contribute to cell proliferation (FLT3, c-KIT, RAS, protein tyrosine standard phosphatase nonreceptor 11); (2) mutations affecting genes involved in myeloid differentiation (AML1 and CEBPA) and (3) mutations affecting genes implicated in cell cycle regulation or apoptosis (P53, NPM1). This nonexhaustive review aims to show how gene mutations interact with each other, how they contribute to refine prognosis and how they can be useful for risk-adapted therapeutic management of AML patients.

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“…Indeed, RUNX1 mutations have frequently been identified in patients with MDS and AML [6,7]. Furthermore, a higher frequency of RUNX1 mutations (30-50%) has been reported in therapyrelated and radiation-associated MDS and AML [13][14][15]. In general, RUNX1 mutations are considered to result in the loss of RUNX1 functions.…”

Section: Abstract Runx1 · Fpd/aml · Fpd/mm · Germ Line Mutationmentioning

confidence: 99%

Myeloid neoplasms with germ line RUNX1 mutation

et al. 2017

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High incidence of somatic mutations in the AML1/RUNX1 gene in myelodysplastic syndrome and low blast percentage myeloid leukemia with myelodysplasia

Cited by 256 publications

References 31 publications

C-terminal mutation of RUNX1 attenuates the DNA-damage repair response in hematopoietic stem cells

C-terminal mutation of RUNX1 attenuates the DNA-damage repair response in hematopoietic stem cells

Cooperating gene mutations in acute myeloid leukemia: a review of the literature

Myeloid neoplasms with germ line RUNX1 mutation

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