Outcome and lineage involvement in t(12;21) childhood acute lymphoblastic leukaemia

Lucchesi, Carlo; Volpe, Gisella; Basso, Giuseppe; Gottardi, Enrico; Barisone, Elena; Spínelli, Mônica Glória Neumann; Ricotti, Emanuela; Cilli, Vania; Perfetto, Fatima; Madon, E; Saglio, Giuseppe

doi:10.1046/j.1365-2141.1997.312676.x

Cited by 27 publications

(12 citation statements)

References 6 publications

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“…The high frequency of myeloid antigen expression (i.e. CD 13 ^nd/or CD33) that was reported originally in a large series of children with ETV6-AML1 rearrangement enrolled in the German and Italian miilticentre trials was confirmed by other reports [177][178][179]. It is interesting to note that other characteristic immunophenotypic features have been described recently that are highly predictive of ETV6-AML1 rearrangement and may be implemented as a screening test for this genetic 'abnormality [296].…”

Section: B Lineage Allmentioning

confidence: 72%

Immunophenotyping of Acute Leukaemias. Immunophänotypisierung akuter Leukämien

Benter¹,

Ratei²,

Wd³

2001

LaboratoriumsMedizin

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For nearly 100 years the classification of blood cells and the diagnosis of leukaemia have been based on cytomorphological features after staining. Even in the era of molecular biology this is still essential. Therapy of acute myeloid leukaemia (AML) is mostly dependent on the interpretation of the morphological appearance of blasts under the microscope. Cytomorphology should also lead to a rational use of techniques like immunophenotyping, cytogenetics, fluorescence / situ hybridisation (FISH), and polymerase chain reaction (PCR).In the past two decades, the impact of immunophenotyping by flow cytometry in the diagnosis and management of acute leukaemia has expanded rapidly. This has been mainly attributed to significant advances in laser and computer technologies and the production of several hundred monoclonal antibodies (moAbs) to a variety of antinens expressed by haematopoietic cells.This review concentrates on immunophenotyping of cells from patients with acute leukaemia and shows the clinical impact on diagnostics and treatment.

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Section: B Lineage Allmentioning

confidence: 72%

Immunophenotyping of Acute Leukaemias. Immunophänotypisierung akuter Leukämien

Benter¹,

Ratei²,

Wd³

2001

LaboratoriumsMedizin

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“…& Alexander, G.J.M. (1997) We read with interest the recent report by Lanza et al (1997) relating to the poor outcome of two of their 11 TEL/AML1positive patients. Here we describe a child with relapsed acute lymphoblastic leukaemia (ALL), TEL/AML1 transcript and p16 homozygous deletion.…”

Section: Department Of Haematologymentioning

confidence: 99%

“…Rearrangement of the TEL and AML1 genes has been associated with excellent prognosis (Shurtleff et al, 1995). Nevertheless, recently some TEL/AML1-positive patients with an extremely adverse prognosis have been detected (Lanza et al, 1997). This could be related to the presence of additional molecular lesions.…”

Section: Department Of Haematologymentioning

confidence: 99%

“…The TEL/AML1 fusion has been described in the B-precursor lineage ALL. Some cases have been published with a hybrid immunophenotype (Cayuela et al, 1996;Lanza et al, 1997), and the case described here corresponds to another The same filter dehybridized and rehybridized with the p16 probe. The case described (lane 3) shows very weak hybridizing bands compared with bands detected after probing with B859.…”

Section: Department Of Haematologymentioning

confidence: 99%

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Correspondence

1997

Br J Haematol

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“…Initially, it was suggested that therapy in this group of patients was so successful that relapse never occurred (Shurtleff et al, 1995;Cayuela et al, 1996;McLean et al, 1996). Nevertheless, more recent studies have shown that relapses do occur Harbott et al, 1997;Lanza et al, 1997;Loh et al, 1998).…”

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confidence: 99%

Minimal residual disease studies are beneficial in the follow‐up of TEL/AML1 patients with B‐precursor acute lymphoblastic leukaemia

et al. 2000

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Summary. The t(12;21)(p13;q22) translocation has been identified as the most common chromosomal abnormality in childhood acute lymphoblastic leukaemia (ALL). Initially, several investigators reported an excellent prognosis in paediatric leukaemias with this translocation, but other studies showed a 20% incidence in relapsed ALL. We performed an extensive analysis of 90 ALL patients. In 17 (19%) cases a TEL/AML1 fusion was found. However, this group was not representative as it included a high number of relapsed patients compared with the normal incidence in B-precursor ALL [54 in continuous complete remission (CCR) and 36 relapsed patients] and only a slightly better prognosis for TEL/AML1-positive patients was found (not significant) (four relapses in 17 TEL/AML1-postive patients vs. 32 relapses in 73 TEL/AML1-negative patients).Comparison of known prognostic factors (age, sex, ploidy, white blood cell count and immunophenotype) between relapsed TEL/AML1-positive and TEL/AML1-positive patients in CCR did not reveal differences, except that the white blood cell count was significantly higher in the relapsed group (P 0´001). Time between diagnosis and relapse was not different for the relapsed TEL/AML1-positive group vs. the relapsed TEL/AML1-negative group. In 11 TEL/AML1-positive patients, the minimal residual disease (MRD) level at the end of induction therapy was quantified in a limiting dilution assay using IGH or TCRD junctional regions as polymerase chain reaction (PCR) targets. In all four relapsed patients, the level of MRD at the end of induction therapy was high (range 0´24±1´2%), whereas in all seven CCR patients, the MRD level was extremely low (0´02 to , 0´001%). In agreement with previous studies in which MRD levels at the end of induction therapy were found to be the strongest risk factor independent of other risk factors, in the present study we show that the MRD level remains a risk factor independent of the presence of a TEL/ AML1 fusion gene.

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Outcome and lineage involvement in t(12;21) childhood acute lymphoblastic leukaemia

Cited by 27 publications

References 6 publications

Immunophenotyping of Acute Leukaemias. Immunophänotypisierung akuter Leukämien

Immunophenotyping of Acute Leukaemias. Immunophänotypisierung akuter Leukämien

Correspondence

Minimal residual disease studies are beneficial in the follow‐up of TEL/AML1 patients with B‐precursor acute lymphoblastic leukaemia

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