Identification of a novel fusion gene <i>MLL‐MAML2</i> in secondary acute myelogenous leukemia and myelodysplastic syndrome with inv(11)(q21q23)

Nemoto, Noriko; Suzukawa, Kazumi; Shimizu, Seiichi; Shinagawa, Atsushi; Takei, Nobuo; Taki, Tomohiko; Hayashi, Yasuhide; Kojima, Hiroshi; Kawakami, Yasushi; Nagasawa, Toshiro

doi:10.1002/gcc.20467

Cited by 40 publications

(40 citation statements)

References 25 publications

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“…2 Fusions between MLL and MAML2 have recently been reported for two adult leukemia patients with secondary AML and myelodysplastic syndrome. 3 Here, we describe the development of secondary T-cell acute lymphoblastic leukemia (T-ALL) in two adolescent leukemia patients. Therapy-related ALL (t-ALL) was diagnosed in a 13-year-old boy 20 months after cessation of treatment for primary AML FAB-M4 Eo.…”

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confidence: 99%

Inv(11)(q21q23) fuses MLL to the Notch co-activator mastermind-like 2 in secondary T-cell acute lymphoblastic leukemia

et al. 2008

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confidence: 99%

Inv(11)(q21q23) fuses MLL to the Notch co-activator mastermind-like 2 in secondary T-cell acute lymphoblastic leukemia

et al. 2008

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“…This translocation has been recurrently found in salivary gland tumors, mucoepidermoid carcinoma, Warthin tumor, and clear cell hidradenoma of the skin. In AML and MDS patients, MLL-MAML2 fusions have been described (39). This fusion disrupts NOTCH signaling and that possibly contributes to carcinogenesis in these malignancies.…”

Section: Discussionmentioning

confidence: 99%

Mastermind-Like 3 Controls Proliferation and Differentiation in Neuroblastoma

Heynen

Nevedomskaya

Palit

et al. 2016

Molecular Cancer Research

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Neuroblastoma cell lines can differentiate upon treatment with retinoic acid (RA), a finding that provided the basis for the clinical use of RA to treat neuroblastoma. However, resistance to RA is often observed, which limits its clinical utility. Using a gain-of-function genetic screen, we identified an unexpected link between RA signaling and mastermindlike 3 (MAML3), a known transcriptional coactivator for NOTCH. Our findings indicate that MAML3 expression leads to the loss of activation of a subset of RA target genes, which hampers RA-induced differentiation and promotes resistance to RA. The regulatory DNA elements of this subset of RA target genes show overlap in binding of MAML3 and the RA receptor, suggesting a direct role for MAML3 in the regulation of these genes. In addition, MAML3 has RA-independent functions, including the activation of IGF1R and downstream AKT signaling via upregulation of IGF2, resulting in increased proliferation. These results demonstrate an important mechanistic role for MAML3 in proliferation and RA-mediated differentiation.Implications: MAML3 coordinates transcription regulation with receptor tyrosine kinase pathway activation, shedding new light on why this gene is mutated in multiple cancers.

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“…In these reports, no data were provided on additional genetic abnormalities that might have contributed to leukemogenesis (Leblanc et al, 1994;Megonigal et al, 2000;Blanco et al, 2001;Metzler et al, 2004;Ng et al, 2004;Takei et al, 2006;Nemoto et al, 2007;Metzler et al, 2008). In the case of secondary myelodysplastic syndrome (MDS) with MLL/FRYL fusion (Robinson et al, 2008), a subclonal presence of t(2;9) was detected in 0-6/20 mitoses in some samples preceding the secondary MDS and loss of chromosome 16 and add (18q) were shown 3 months before the evident secondary MDS diagnosis in 4 out of 17 t(4;11) positive cells.…”

Section: Discussionmentioning

confidence: 99%

“…In these cases the MLL positive cells characteristic for the secondary malignancy were described as progressively expanding clone finally prevailing over the normal hematopoiesis causing clinical symptoms of leukemia. On the contrary, Japanese group detected an inv(11)(q21;q23) with MLL/MAML2 fusion almost 6 years before the secondary AML onset (Takei et al, 2006;Nemoto et al, 2007). Two cases describing treatment related MLL translocation were published recently.…”

Section: Discussionmentioning

confidence: 99%

“…The majority of secondary or treatment related leukemias with MLL gene rearrangements are also characterized by a relatively short latency (Felix, 1998). On the other hand, in a few cases of secondary hematological malignancies with MLL gene fusions, it has been possible to backtrack the appearance of the MLL rearrangement to several months (up to more than 6 years) prior to diagnosis of secondary leukemia (Leblanc et al, 1994;Megonigal et al, 2000;Blanco et al, 2001;Metzler et al, 2004;Ng et al, 2004;Takei et al, 2006;Nemoto et al, 2007;Metzler et al, 2008;Robinson et al, 2008) (see Table 1). We report here a case of secondary, B-lineage acute lymphoblastic leukemia (ALL) with MLL/ FOXO3A fusion gene.…”

Section: Introductionmentioning

confidence: 99%

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Covert preleukemia driven by MLL gene fusion

Zuna

Burjanivová

Mejstříková

et al. 2008

Genes Chromosomes & Cancer

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Acute leukemia is considered to be a two-or multiple-step process. Although there is a considerable knowledge regarding the character of the ''first hit,'' the nature of the ''second hit'' remains unanswered in most of the cases including leukemias with MLL gene rearrangement. We demonstrate here a striking sequence of events, which include a covert, protracted preleukemic phase characterized by a dominant MLL/FOXO3A clone with intact myeloid differentiation and the subsequent acquisition of a secondary genetic abnormality, leading to overt lymphoblastic leukemia. Backtracking of the secondary acute lymphoblastic leukemia (sALL) with the MLL rearrangement showed no blasts in the bone marrow (BM) during the protracted preleukemic phase. However, at the same time (more than 1 year before the sALL diagnosis) the MLL/FOXO3A was present in up to 90% of BM cells including myeloid lineage, suggesting that the fusion arose in a multipotent progenitor. To identify potential ''second hit'' precipitating sALL we compared DNA in preleukemic versus fully leukemic samples. The analysis revealed a 10 Mb gain on 19q13.32 in the sALL, absent in the preleukemic specimen. These data provide insight into the dynamics of leukemogenesis in secondary leukemia with MLL rearrangement.

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Identification of a novel fusion gene MLL‐MAML2 in secondary acute myelogenous leukemia and myelodysplastic syndrome with inv(11)(q21q23)

Cited by 40 publications

References 25 publications

Inv(11)(q21q23) fuses MLL to the Notch co-activator mastermind-like 2 in secondary T-cell acute lymphoblastic leukemia

Inv(11)(q21q23) fuses MLL to the Notch co-activator mastermind-like 2 in secondary T-cell acute lymphoblastic leukemia

Mastermind-Like 3 Controls Proliferation and Differentiation in Neuroblastoma

Covert preleukemia driven by MLL gene fusion

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