Risk-adapted postremission therapy in acute myeloid leukemia: results of the german multicenter AML HD93 treatment trial

Schlenk, Richard F.; Benner, Axel; Hartmann, Frank; Valle, Francisco del; Weber, Claudia; Pralle, H.; Fischer, J. Th.; Gunzer, U; Pezzutto, Antonio; Weber, Walter; Grimminger, W; Preiß, Joachim; Hensel, Manfred; Fröhling, Stefan; Döhner, Konstanze; Haas, Rainer; Döhner, Hartmut

doi:10.1038/sj.leu.2403009

Cited by 106 publications

(82 citation statements)

References 43 publications

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“…28 The cytogenetically defined risk classification of AML may also have an impact in designing a treatment trial in AML by risk-adapted postremission therapy. 29 In the present series, by using various molecular technology in addition to conventional cytogenetic analysis, we identified that 47.9% (56/ 117) of patients had the four major recurrent genetic abnormalities of AML1-ETO, CBFb-MYH11, PML-RARa and MLL rearrangements defined by the WHO classification. 15 However, approximately half of children with AML have no chromosomal or genetic abnormalities that can predict outcome, efforts have been made to improve the prognostic stratification on this group of patients.…”

Section: Discussionmentioning

confidence: 99%

CEBPα mutations in childhood acute myeloid leukemia

et al. 2004

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CEBPa mutations have been described in adult acute myeloid leukemia (AML) and conferred a favorable prognosis. However, CEBPa mutation has not been reported in children. We investigated 117 children with de novo AML using DNA PCR assay followed by sequencing for each PCR product. CEBPa mutations were detected in seven patients, four had FAB M2, two M1 and one M4. CEBPa mutations only occurred in patients with intermediate cytogenetics and not in 56 children with AML1-ETO, CBFb-MYH11, PML-RARa or MLL rearrangements. Five patients had mutations occurred in both N-terminal part and basic-leucine zipper (bZIP) domain, one had an N-terminal frameshift mutation and the remaining one had an inframe insertion in the bZIP domain. Cloning analysis on five samples carrying more than one mutations demonstrated one homozygous combined mutations and four heterozygous biallelic mutations. Four of seven CEBPa mutation( þ ) patients had cooperating mutations with FLT3-ITD or N-ras mutations compared to 27 in 109 CEBPa mutation(À) patients. Our results showed that CEBPa mutations occurred in 6% of childhood AML and most exhibited combined mutations in both Nterminal part and bZIP domain.

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Section: Discussionmentioning

confidence: 99%

CEBPα mutations in childhood acute myeloid leukemia

et al. 2004

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“…Prognostic factors of relapse risk in CBFb-AML subset are still a matter of debate. Female gender, older age, and low-platelet count have been reported as predictors for inferior outcome and/or shorter disease-free survival in patients enrolled in prospective trials [1,17,18]. Furthermore, higher white blood cells (WBCs) and low-platelet counts have been identified as bad predictor factors for CR achievements [19,20].…”

Section: Introductionmentioning

confidence: 99%

Old and new prognostic factors in acute myeloid leukemia with deranged core‐binding factor beta

et al. 2013

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Acute myeloid leukemia (AML) with deranged core‐binding factor beta (CBFβ) is usually associated with a favorable prognosis with 50–70% of patients cured using contemporary treatments. We analyzed the prognostic significance of clinical features on 58 patients with CBFβ‐AML aged ≤60 years. Increasing age was the only predictor for survival (P <0.001), with an optimal cut‐point at 43 years. White blood cells (WBCs) at diagnosis emerged as an independent risk factor for relapse incidence (P = 0.017), with 1.1% increase of hazard for each 1.0 × 109/L WBC increment. KIT mutations lacked prognostic value for survival and showed only a trend for relapse incidence (P = 0.069). Am. J. Hematol. 88:594–600, 2013. © 2013 Wiley Periodicals, Inc.

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“…Fourthly, all of the clinical trials have been characterized by lack of compliance with the assigned treatment. 13 As shown in Table 2, only 70% of patients in four of the large studies actually received an HLAidentical sibling transplant. Moreover, less than 50% of patients available for randomization to autologous BMT or conventional chemotherapy were randomized and less than 70% of patients assigned to receive autografts actually received them.…”

Section: Limitations Of Clinical Trial Datamentioning

confidence: 99%

The role of allogeneic transplantation in high-risk acute myelogenous leukemia

Drobyski

2004

Leukemia

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Patients with high-risk acute myelogenous leukemia (AML) in first remission are at increased risk for disease recurrence and are often considered for allogeneic bone marrow transplantation (BMT) if there is a suitable HLA-identical sibling donor. Analysis of results from randomized clinical trials comparing different treatment strategies for patients with AML (chemotherapy, autologous BMT, and allogeneic BMT) suggests that allogeneic BMT may be a superior treatment modality for patients in the high-risk subgroup. Interpretation of clinical trial results, however, is problematic due to poor compliance with transplant options, absence of studies specifically designed to addresses this question, and ongoing redefinition of the highrisk subgroup. Alternative allogeneic transplant approaches to reduce toxicity from graft-versus-host disease and enhance graft-versus-leukemia reactivity may offer therapeutic promise in this patient population.

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Risk-adapted postremission therapy in acute myeloid leukemia: results of the german multicenter AML HD93 treatment trial

Cited by 106 publications

References 43 publications

CEBPα mutations in childhood acute myeloid leukemia

CEBPα mutations in childhood acute myeloid leukemia

Old and new prognostic factors in acute myeloid leukemia with deranged core‐binding factor beta

The role of allogeneic transplantation in high-risk acute myelogenous leukemia

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