Landscape of driver mutations and their clinical impacts in pediatric B-cell precursor acute lymphoblastic leukemia

Ueno, Hikaru; Yoshida, Kenichi; Shiozawa, Yusuke; Nannya, Yasuhito; Iijima-Yamashita, Yuka; Kiyokawa, Nobutaka; Shiraishi, Yuichi; Chiba, Kenichi; Tanaka, Hiroko; Isobe, Tomoya; Seki, Masafumi; Kimura, Shunsuke; Makishima, Hideki; Nakagawa, Masahiro; Kakiuchi, Nobuyuki; Kataoka, Keisuke; Nishijima, Dai; Deguchi, Takao; Ohki, Kentaro; Satō, Atsushi; Takahashi, Hiroyuki; Hashii, Yoshiko; Tokimasa, Sadao; Hara, Junichi; Kosaka, Yoshiyuki; Kato, Koji; Inukai, Takeshi; Takita, Junko; Imamura, Toshihiko; Miyano, Satoru; Manabe, Atsushi; Horibe, Keizo; Ogawa, Seishi; Sanada, Masashi

doi:10.1182/bloodadvances.2019001307

Cited by 38 publications

(36 citation statements)

References 31 publications

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“…MEF2D (myocyte enhancer factor 2D) rearrangements occur in ~4% of childhood and 10% adult B-ALL cases. This subtype shows a distinct immunophenotype with low/absent expression of CD10, and positivity for CD38 and cytoplasmic µ chain, and distinct expression profiles [7,[85][86][87][88]. MEF2D is the 5 partner in all described fusions, whereas B-cell CLL/lymphoma (BCL) 9 and heterogeneous nuclear ribonucleoprotein U-like 1 (HNRNPUL1) are the two most recurrent 3 partners.…”

Section: Dux4 Mef2d Znf384 and Nutm1 Gene Fusionsmentioning

confidence: 99%

“…NUTM1 (nuclear protein in testis midline carcinoma family 1) rearrangements (<2% of childhood B-ALL and mostly infant without KMT2A-rearrangements) [7,13,88,[98][99][100] are characterized by fusion of NUTM1 to different partners, including transcription factors and epigenetic regulators (e.g., ACIN1, AFF1, ATAD5, BRD9, CHD4, CUX1, IKZF1, RUNX1, SLC12A6, and ZNF618), that drive aberrant NUTM1 expression [7,13]. In all fusions, the NUT domain is retained, and this is hypothesized to lead to global changes in chromatin acetylation [101] and to sensitivity to histone deacetylase inhibitors or bromodomain inhibitors in case of fusions with BRD9.…”

Section: Dux4 Mef2d Znf384 and Nutm1 Gene Fusionsmentioning

confidence: 99%

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Biologic and Therapeutic Implications of Genomic Alterations in Acute Lymphoblastic Leukemia

Iacobucci

Kimura

Mullighan

2021

JCM

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Acute lymphoblastic leukemia (ALL) is the most successful paradigm of how risk-adapted therapy and detailed understanding of the genetic alterations driving leukemogenesis and therapeutic response may dramatically improve treatment outcomes, with cure rates now exceeding 90% in children. However, ALL still represents a leading cause of cancer-related death in the young, and the outcome for older adolescents and young adults with ALL remains poor. In the past decade, next generation sequencing has enabled critical advances in our understanding of leukemogenesis. These include the identification of risk-associated ALL subtypes (e.g., those with rearrangements of MEF2D, DUX4, NUTM1, ZNF384 and BCL11B; the PAX5 P80R and IKZF1 N159Y mutations; and genomic phenocopies such as Ph-like ALL) and the genomic basis of disease evolution. These advances have been complemented by the development of novel therapeutic approaches, including those that are of mutation-specific, such as tyrosine kinase inhibitors, and those that are mutation-agnostic, including antibody and cellular immunotherapies, and protein degradation strategies such as proteolysis-targeting chimeras. Herein, we review the genetic taxonomy of ALL with a focus on clinical implications and the implementation of genomic diagnostic approaches.

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Section: Dux4 Mef2d Znf384 and Nutm1 Gene Fusionsmentioning

confidence: 99%

Section: Dux4 Mef2d Znf384 and Nutm1 Gene Fusionsmentioning

confidence: 99%

Biologic and Therapeutic Implications of Genomic Alterations in Acute Lymphoblastic Leukemia

Iacobucci

Kimura

Mullighan

2021

JCM

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“…The different RAS signaling alterations have been shown to be mutually exclusive, suggesting that, in contrast to the convergent evolution for RAS mutations observed in infants with MLL-rearranged B-ALL [ 52 ], a single alteration in the pathway is sufficient to maintain constitutive RAS-pathway activation. Focal deletions or point mutations in NF1 gene are the most recurrent genetic alterations of near-haploid B-ALL (≥44% of patients) [ 23 , 30 , 53 ]. NF1 encodes a RAS–GTPase-activating protein that negatively regulates Ras signaling.…”

Section: Molecular Characterization Of Hypodiploid B-all With <40 Chromosomesmentioning

confidence: 99%

“…A recent study by the Japan Association Childhood Leukemia Study Group (JACLS) reported a high frequency of mutations in CIC in both low-hypodiploid and near-haploid B-ALL, present in 5 of 9 patients [ 53 ]. CIC is a member of the high mobility group (HMG)-box superfamily of transcriptional repressors and is recurrently mutated in oligodendrogliomas and in round cell sarcomas.…”

Section: Molecular Characterization Of Hypodiploid B-all With <40 Chromosomesmentioning

confidence: 99%

“…CIC is a member of the high mobility group (HMG)-box superfamily of transcriptional repressors and is recurrently mutated in oligodendrogliomas and in round cell sarcomas. However, the germline status of CIC in B-ALL with hypodiploidy of <40 chromosomes is unknown and raises the question of whether it could be more prevalent in Asian ancestors than in non-Asian populations [ 53 ].…”

Section: Molecular Characterization Of Hypodiploid B-all With <40 Chromosomesmentioning

confidence: 99%

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Near-Haploidy and Low-Hypodiploidy in B-Cell Acute Lymphoblastic Leukemia: When Less Is Too Much

Molina

Bataller

Thampi

et al. 2021

Cancers

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Hypodiploidy with less than 40 chromosomes is a rare genetic abnormality in B-cell acute lymphoblastic leukemia (B-ALL). This condition can be classified based on modal chromosome number as low-hypodiploidy (30–39 chromosomes) and near-haploidy (24–29 chromosomes), with unique cytogenetic and mutational landscapes. Hypodiploid B-ALL with <40 chromosomes has an extremely poor outcome, with 5-year overall survival rates below 50% and 20% in childhood and adult B-ALL, respectively. Accordingly, this genetic feature represents an adverse prognostic factor in B-ALL and is associated with early relapse and therapy refractoriness. Notably, half of all patients with hypodiploid B-ALL with < 40 chromosomes cases ultimately exhibit chromosome doubling of the hypodiploid clone, resulting in clones with 50–78 chromosomes. Doubled clones are often the major clones at diagnosis, leading to “masked hypodiploidy”, which is clinically challenging as patients can be erroneously classified as hyperdiploid B-ALL. Here, we summarize the main cytogenetic and molecular features of hypodiploid B-ALL subtypes, and provide a brief overview of the diagnostic methods, standard-of-care treatments and overall clinical outcome. Finally, we discuss molecular mechanisms that may underlie the origin and leukemogenic impact of hypodiploidy and may open new therapeutic avenues to improve survival rates in these patients.

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The clinical outcomes and genomic landscapes of acute lymphoblastic leukemia patients with E2A‐PBX1: A 10‐year retrospective study

et al. 2021

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The clinical outcomes and genomic features of E2A‐PBX1 (TCF3‐PBX1)‐positive B‐cell acute lymphoblastic leukemia (B‐ALL) patients remain unclear. A total of 137 patients carrying E2A‐PBX1 among 3164 B‐ALL patients between 2009 and 2019 were retrospectively analyzed. The 5‐year overall survival (OS) and disease‐free survival (DFS) rates of the whole cohort were 68.6% and 61.0%, respectively. Age [DFS, p = 0.037; cumulative incidence of relapse (CIR), p = 0.005] and the level of minimal residual disease (MRD) after induction chemotherapy (OS, p = 0.020; DFS, p = 0.002; CIR, p = 0.006) were independent risk factors. In adolescents/adults, allogeneic hematopoietic stem cell transplantation (allo‐HSCT) at first complete remission (CR1) significantly improved the 5‐year prognosis (OS, p < 0.001; DFS, p < 0.001; CIR, p < 0.001). Haploidentical HSCT decreased the CIR compared with human leukocyte antigen‐matched HSCT in adolescents/adults (p = 0.017). Mutations in PBX1, PAX5, CTCF and SETD2, amplification of AKT3, and deletion of CDKN2A/B were common in the total cohort, while transcriptome differences were found in the cell cycle, nerve growth factor (NGF) signaling pathway and transcriptional regulation by TP53 between adolescents/adults and children. Patients with multiple subclones at diagnosis tended to have unfavorable 3‐year prognoses (DFS, p = 0.010; CIR, p = 0.021). Leukemia clones with DNA repair gene mutations showed aggressive and treatment‐refractory phenotypes in this subtype of ALL. Our study indicated that age, the level of MRD and DNA repair gene mutations were associated with E2A‐PBX1‐positive B‐ALL outcomes. Allo‐HSCT, especially haploidentical HSCT, could improve the prognosis of adolescent/adult patients.

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Landscape of driver mutations and their clinical impacts in pediatric B-cell precursor acute lymphoblastic leukemia

Cited by 38 publications

References 31 publications

Biologic and Therapeutic Implications of Genomic Alterations in Acute Lymphoblastic Leukemia

Biologic and Therapeutic Implications of Genomic Alterations in Acute Lymphoblastic Leukemia

Near-Haploidy and Low-Hypodiploidy in B-Cell Acute Lymphoblastic Leukemia: When Less Is Too Much

The clinical outcomes and genomic landscapes of acute lymphoblastic leukemia patients with E2A‐PBX1: A 10‐year retrospective study

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