Mutation of Genes Affecting the RAS Pathway Is Common in Childhood Acute Lymphoblastic Leukemia

Case, Marian; Matheson, Elizabeth; Minto, Lynne; Hassan, Rosline; Harrison, Christine J.; Bown, Nick; Bailey, Simon; Vormoor, Josef; Hall, Andrew G.; Irving, Julie

doi:10.1158/0008-5472.can-08-0101

Cited by 125 publications

(153 citation statements)

References 35 publications

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“…Whether these are caused by the previous genotoxic therapy or are a consequence of inherent clonal evolution over time is unknown, and may well be impossible to clarify because ALL treatment is solely based on chemotherapy. However, it should be stressed that Case et al 28 showed that, using standard PCR and denaturing high performance liquid chromatography, RTK-RAS mutations may seem to arise at relapse; however, highly sensitive allele-specific PCR analyses nevertheless may identify them already at diagnosis, suggesting the presence of the clone that later relapsed already at the time of diagnosis.…”

Section: Discussionmentioning

confidence: 99%

Relapsed childhood high hyperdiploid acute lymphoblastic leukemia: presence of preleukemic ancestral clones and the secondary nature of microdeletions and RTK-RAS mutations

et al. 2010

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Although childhood high hyperdiploid acute lymphoblastic leukemia is associated with a favorable outcome, 20% of patients still relapse. It is important to identify these patients already at diagnosis to ensure proper risk stratification. We have investigated 11 paired diagnostic and relapse samples with single nucleotide polymorphism array and mutation analyses of FLT3, KRAS, NRAS and PTPN11 in order to identify changes associated with relapse and to ascertain the genetic evolution patterns. Structural changes, mainly cryptic hemizygous deletions, were significantly more common at relapse (Po0.05). No single aberration was linked to relapse, but four deletions, involving IKZF1, PAX5, CDKN2A/B or AK3, were recurrent. On the basis of the genetic relationship between the paired samples, three groups were delineated: (1) identical genetic changes at diagnosis and relapse (2 of 11 cases), (2) clonal evolution with all changes at diagnosis being present at relapse (2 of 11) and (3) clonal evolution with some changes conserved, lost or gained (7 of 11), suggesting the presence of a preleukemic clone. This ancestral clone was characterized by numerical changes only, with structural changes and RTK-RAS mutations being secondary to the high hyperdiploid pattern.

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Section: Discussionmentioning

confidence: 99%

Relapsed childhood high hyperdiploid acute lymphoblastic leukemia: presence of preleukemic ancestral clones and the secondary nature of microdeletions and RTK-RAS mutations

et al. 2010

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“…The present finding that deletions of SPRED1 are recurrent and that they provide a negative prognostic impact in BCP ALL is clinically important, not least considering that SPRED1 is part of MAPK signaling and that inhibitors of this pathway currently are undergoing clinical trials and hence may be novel therapeutic options. 24 The multivariate analyses strongly indicated that IKZF1 deletions were the strongest independent risk factor for poor outcome ( Table 4). The transcription factor IKZF1 is essential for B-cell development, with loss of IKZF1 leading to arrest of lymphoid differentiation.…”

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confidence: 94%

“…22,23 SPRED1 has previously not been implicated in ALL but mutations of other RTK-RAS genes, such as FLT3, KRAS, NRAS, and PTPN11, have been reported to be enriched at ALL relapses. 16,24 The only genomic imbalance significantly associated with relapse (Table 2) was del(6)(p22.2p22.2), involving the histone genes HIST1H2BD and HIST1H1E in the smallest overlapping region. HIST1H2BD and HIST1H1E are part of the nucleosome structure of the chromosomal fiber and essential for cytokinesis.…”

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confidence: 99%

Deletions of IKZF1 and SPRED1 are associated with poor prognosis in a population-based series of pediatric B-cell precursor acute lymphoblastic leukemia diagnosed between 1992 and 2011

et al. 2013

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, Castor, A., Behrendtz, M., Biloglav, A., Forestier, E., Paulsson, K., & Johansson, B. (2014). Deletions of IKZF1 and SPRED1 are associated with poor prognosis in a population-based series of pediatric B-cell precursor acute lymphoblastic leukemia diagnosed between 1992 and 2011. Leukemia, 28(2), 302-310. DOI: 10.1038DOI: 10. /leu.2013 General rights Copyright and moral rights for the publications made accessible in the public portal are retained by the authors and/or other copyright owners and it is a condition of accessing publications that users recognise and abide by the legal requirements associated with these rights.• Users may download and print one copy of any publication from the public portal for the purpose of private study or research.• You may not further distribute the material or use it for any profit-making activity or commercial gain • You may freely distribute the URL identifying the publication in the public portal and TBL1XR1 were significantly more common in B-cell precursor ALL patients who relapsed compared with those remaining in complete remission. In univariate analyses, age (≥10 years), WBC counts (>100 x 10 9 /l), t(9;22)(q34;q11), MLL rearrangements, nearhaploidy, and deletions of ATP10A, IKZF1, SPRED1, and the pseudoautosomal 1 regions on Xp/Yp were significantly associated with decreased 10-year event-free survival, with IKZF1 abnormalities being an independent risk factor in multivariate analysis irrespective of risk group. High age and deletions of IKZF1 and SPRED1 were also associated with poor overall survival. Thus, analyses of these genes provide clinically important information.

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“…In particular we tested for a BCR-ABL1-like expression signature including specific targetable fusions, 4 performed phospho-flow cytometry for targetable kinase activity; low-density genomic analysis by multiplex ligation-dependent PCR (MLPA); and screened for activating RAS or JAK mutations. 4,5 Twenty non-irradiated, immune-deficient, NOD/SCID/IL-2 receptor gamma − / − (NOD.Cg-Prkdc scid Il2rg tm1Wjl /SzJ, NSG) mice were inoculated by tail vein injection 8 days after the 2nd relapse with 2 × 10 6 BM cells (from the 2nd relapse) to establish the PDX. 6 1.0E-01 Following a 2nd course of topotecan, MRD was undetectable 119 days after the 2nd relapse and remained negative until 259 days after the 2nd relapse.…”

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confidence: 99%

“…MLPA analysis showed heterozygous deletion of JAK2 exon 23, homozygous deletion of CDNK2A and B, and diploid copy number for EBF1, IKZF1, PAX5, ETV6, BTG1, RB1 and CRLF2 (Supplementary Table S3). The targeted analyses were negative for the known KRAS or NRAS mutations 5 and negative for fusions and mutations in JAK1 and JAK2. 4 Gene expression profiling for a BCR-ABL1-like signature showed no overexpression of CRLF2, PDGFRB, ABL1, ABL2 or EPOR.…”

mentioning

confidence: 99%

Xenograft-directed personalized therapy for a patient with post-transplant relapse of ALL

Trahair

Lock²,

Sutton³

et al. 2016

Bone Marrow Transplant

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Mutation of Genes Affecting the RAS Pathway Is Common in Childhood Acute Lymphoblastic Leukemia

Cited by 125 publications

References 35 publications

Relapsed childhood high hyperdiploid acute lymphoblastic leukemia: presence of preleukemic ancestral clones and the secondary nature of microdeletions and RTK-RAS mutations

Relapsed childhood high hyperdiploid acute lymphoblastic leukemia: presence of preleukemic ancestral clones and the secondary nature of microdeletions and RTK-RAS mutations

Deletions of IKZF1 and SPRED1 are associated with poor prognosis in a population-based series of pediatric B-cell precursor acute lymphoblastic leukemia diagnosed between 1992 and 2011

Xenograft-directed personalized therapy for a patient with post-transplant relapse of ALL

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