Translocation t(2;3)(p15-23;q26-27) in myeloid malignancies: Report of 21 new cases clinical, cytogenetic and molecular genetic features

M. Stevens-Kroef; B. Poppe; S. van Zelderen-Bhola; E. van den Berg; M. van der Blij-Philipsen; A. Geurts van Kessel; R. Slater; G. Hamers; L. Michaux; F. Speleman; Anne Hagemeijer

doi:10.1038/sj.leu.2403346

Translocation t(2;3)(p15-23;q26-27) in myeloid malignancies: Report of 21 new cases clinical, cytogenetic and molecular genetic features

M. Stevens-Kroef, B. Poppe, S. van Zelderen-Bhola, E. van den Berg, M. van der Blij-Philipsen, A. Geurts van Kessel, R. Slater, G. Hamers, L. Michaux, F. Speleman, Anne Hagemeijer^*

^*Corresponding author for this work

Human genetics

Research output: Contribution to journal › Review article › Academic › peer-review

Abstract

Chromosomal rearrangements involving 3q26 either due to inversion or translocation with various partner chromosomes are a recurrent finding in malignant myeloid disorders. Typically, these chromosome aberrations contribute to ectopic expression of or to the formation of fusion genes involving the EVI1 proto-oncogene. Chromosomal translocations involving the short arm of chromosome 2 (p15-p23) and the distal part of the long arm of chromosome 3 (q26-q27) are a rare but recurrent finding in patients with myeloid malignancies, and are assumed to be part of this spectrum of disorders. Thus far, however, these translocations have been poorly studied. Here, we present 21 new cases with myelodysplasia, acute myeloid leukemia or CML in blast crisis, which upon karyotyping showed the presence of a t(2;3). Furthermore, an extensive literature review disclosed 29 additional cases. Morphological, clinical and cytogenetic assessment revealed the typical hallmarks of 3q26/EVI1 rearrangements, that is, trilineage dysplasia and dysmegakaryopoiesis, poor progriosis and additional monosomy 7. Molecular cytogenetic analysis and PCR in selected samples indicated that in most cases the translocation indeed targets the EVI1 locus. Mapping of the chromosome 2 breakpoints confirmed the initially suspected cytogenetic breakpoint heterogeneity at the 2p arm.

Original language	English
Pages (from-to)	1108-1114
Number of pages	7
Journal	Leukemia
Volume	18
Issue number	6
DOIs	https://doi.org/10.1038/sj.leu.2403346
Publication status	Published - Jun 2004

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Stevens-Kroef, M., Poppe, B., van Zelderen-Bhola, S., van den Berg, E., van der Blij-Philipsen, M., Geurts van Kessel, A., Slater, R., Hamers, G., Michaux, L., Speleman, F., & Hagemeijer, A. (2004). Translocation t(2;3)(p15-23;q26-27) in myeloid malignancies: Report of 21 new cases clinical, cytogenetic and molecular genetic features. Leukemia, 18(6), 1108-1114. https://doi.org/10.1038/sj.leu.2403346

@article{3f9c8f0b36fb4a559f03b020ffe0a1cc,

title = "Translocation t(2;3)(p15-23;q26-27) in myeloid malignancies: Report of 21 new cases clinical, cytogenetic and molecular genetic features",

abstract = "Chromosomal rearrangements involving 3q26 either due to inversion or translocation with various partner chromosomes are a recurrent finding in malignant myeloid disorders. Typically, these chromosome aberrations contribute to ectopic expression of or to the formation of fusion genes involving the EVI1 proto-oncogene. Chromosomal translocations involving the short arm of chromosome 2 (p15-p23) and the distal part of the long arm of chromosome 3 (q26-q27) are a rare but recurrent finding in patients with myeloid malignancies, and are assumed to be part of this spectrum of disorders. Thus far, however, these translocations have been poorly studied. Here, we present 21 new cases with myelodysplasia, acute myeloid leukemia or CML in blast crisis, which upon karyotyping showed the presence of a t(2;3). Furthermore, an extensive literature review disclosed 29 additional cases. Morphological, clinical and cytogenetic assessment revealed the typical hallmarks of 3q26/EVI1 rearrangements, that is, trilineage dysplasia and dysmegakaryopoiesis, poor progriosis and additional monosomy 7. Molecular cytogenetic analysis and PCR in selected samples indicated that in most cases the translocation indeed targets the EVI1 locus. Mapping of the chromosome 2 breakpoints confirmed the initially suspected cytogenetic breakpoint heterogeneity at the 2p arm.",

keywords = "Dysmegakaryopoiesis, EVI1 overexpression, Myeloid malignancies, Poor prognosis, Recurent chromosome abnormality, Translocation t(2;3)",

author = "M. Stevens-Kroef and B. Poppe and {van Zelderen-Bhola}, S. and {van den Berg}, E. and {van der Blij-Philipsen}, M. and {Geurts van Kessel}, A. and R. Slater and G. Hamers and L. Michaux and F. Speleman and Anne Hagemeijer",

note = "Funding Information: We gratefully acknowledge Dr GE Beverstock (Leiden University Medical Centre), Dr WPM Breed (Catharina Hospital Eindhoven), Dr SMGJ Daenen (University Hospital Groningen), Dr JC Kluin-Nelemans (Leiden University Medical Center), Dr P Muus (University Medical Center St Radboud Nijmegen), Dr H Schouten (University Hospital Maastricht), Dr GEG Verhoef (University Hospital Leuven), Dr A Van Hoof (AZ St Jan, Brugge), Dr C Dubois (St Jan, Brussels) and Dr P Zachee (Algemeen Centrum Zieken-huis, Antwerp) for providing all clinical data of their patients, P Meeus and C Brusselmans for review of bone marrow morphology, Josefa Albrechts, Betty Emanuel and Nurten Yigit for technical support and R Logist for help in preparing the paper. This text presents research results of the Belgian program of Interuniversity Poles of attraction initiated by the Belgian State, Prime Minister{\textquoteright}s Office, Science Policy Programming. The scientific responsibility is assumed by the authors. This study was partially supported by the Fund for Scientific Research of Flanders (FWO – Vlaanderen), Grant No. G.0310.01. Bruce Poppe is a research fellow of the Fund for Scientific Research of Flanders.",

year = "2004",

month = jun,

doi = "10.1038/sj.leu.2403346",

language = "English",

volume = "18",

pages = "1108--1114",

journal = "Leukemia",

issn = "0887-6924",

publisher = "Nature Publishing Group",

number = "6",

}

Stevens-Kroef, M, Poppe, B, van Zelderen-Bhola, S, van den Berg, E, van der Blij-Philipsen, M, Geurts van Kessel, A, Slater, R, Hamers, G, Michaux, L, Speleman, F & Hagemeijer, A 2004, 'Translocation t(2;3)(p15-23;q26-27) in myeloid malignancies: Report of 21 new cases clinical, cytogenetic and molecular genetic features', Leukemia, vol. 18, no. 6, pp. 1108-1114. https://doi.org/10.1038/sj.leu.2403346

TY - JOUR

T1 - Translocation t(2;3)(p15-23;q26-27) in myeloid malignancies

T2 - Report of 21 new cases clinical, cytogenetic and molecular genetic features

AU - Stevens-Kroef, M.

AU - Poppe, B.

AU - van Zelderen-Bhola, S.

AU - van den Berg, E.

AU - van der Blij-Philipsen, M.

AU - Geurts van Kessel, A.

AU - Slater, R.

AU - Hamers, G.

AU - Michaux, L.

AU - Speleman, F.

AU - Hagemeijer, Anne

N1 - Funding Information: We gratefully acknowledge Dr GE Beverstock (Leiden University Medical Centre), Dr WPM Breed (Catharina Hospital Eindhoven), Dr SMGJ Daenen (University Hospital Groningen), Dr JC Kluin-Nelemans (Leiden University Medical Center), Dr P Muus (University Medical Center St Radboud Nijmegen), Dr H Schouten (University Hospital Maastricht), Dr GEG Verhoef (University Hospital Leuven), Dr A Van Hoof (AZ St Jan, Brugge), Dr C Dubois (St Jan, Brussels) and Dr P Zachee (Algemeen Centrum Zieken-huis, Antwerp) for providing all clinical data of their patients, P Meeus and C Brusselmans for review of bone marrow morphology, Josefa Albrechts, Betty Emanuel and Nurten Yigit for technical support and R Logist for help in preparing the paper. This text presents research results of the Belgian program of Interuniversity Poles of attraction initiated by the Belgian State, Prime Minister’s Office, Science Policy Programming. The scientific responsibility is assumed by the authors. This study was partially supported by the Fund for Scientific Research of Flanders (FWO – Vlaanderen), Grant No. G.0310.01. Bruce Poppe is a research fellow of the Fund for Scientific Research of Flanders.

PY - 2004/6

Y1 - 2004/6

N2 - Chromosomal rearrangements involving 3q26 either due to inversion or translocation with various partner chromosomes are a recurrent finding in malignant myeloid disorders. Typically, these chromosome aberrations contribute to ectopic expression of or to the formation of fusion genes involving the EVI1 proto-oncogene. Chromosomal translocations involving the short arm of chromosome 2 (p15-p23) and the distal part of the long arm of chromosome 3 (q26-q27) are a rare but recurrent finding in patients with myeloid malignancies, and are assumed to be part of this spectrum of disorders. Thus far, however, these translocations have been poorly studied. Here, we present 21 new cases with myelodysplasia, acute myeloid leukemia or CML in blast crisis, which upon karyotyping showed the presence of a t(2;3). Furthermore, an extensive literature review disclosed 29 additional cases. Morphological, clinical and cytogenetic assessment revealed the typical hallmarks of 3q26/EVI1 rearrangements, that is, trilineage dysplasia and dysmegakaryopoiesis, poor progriosis and additional monosomy 7. Molecular cytogenetic analysis and PCR in selected samples indicated that in most cases the translocation indeed targets the EVI1 locus. Mapping of the chromosome 2 breakpoints confirmed the initially suspected cytogenetic breakpoint heterogeneity at the 2p arm.

AB - Chromosomal rearrangements involving 3q26 either due to inversion or translocation with various partner chromosomes are a recurrent finding in malignant myeloid disorders. Typically, these chromosome aberrations contribute to ectopic expression of or to the formation of fusion genes involving the EVI1 proto-oncogene. Chromosomal translocations involving the short arm of chromosome 2 (p15-p23) and the distal part of the long arm of chromosome 3 (q26-q27) are a rare but recurrent finding in patients with myeloid malignancies, and are assumed to be part of this spectrum of disorders. Thus far, however, these translocations have been poorly studied. Here, we present 21 new cases with myelodysplasia, acute myeloid leukemia or CML in blast crisis, which upon karyotyping showed the presence of a t(2;3). Furthermore, an extensive literature review disclosed 29 additional cases. Morphological, clinical and cytogenetic assessment revealed the typical hallmarks of 3q26/EVI1 rearrangements, that is, trilineage dysplasia and dysmegakaryopoiesis, poor progriosis and additional monosomy 7. Molecular cytogenetic analysis and PCR in selected samples indicated that in most cases the translocation indeed targets the EVI1 locus. Mapping of the chromosome 2 breakpoints confirmed the initially suspected cytogenetic breakpoint heterogeneity at the 2p arm.

KW - Dysmegakaryopoiesis

KW - EVI1 overexpression

KW - Myeloid malignancies

KW - Poor prognosis

KW - Recurent chromosome abnormality

KW - Translocation t(2;3)

UR - http://www.scopus.com/inward/record.url?scp=2942648751&partnerID=8YFLogxK

U2 - 10.1038/sj.leu.2403346

DO - 10.1038/sj.leu.2403346

M3 - Review article

C2 - 15085164

AN - SCOPUS:2942648751

SN - 0887-6924

VL - 18

SP - 1108

EP - 1114

JO - Leukemia

JF - Leukemia

IS - 6

ER -

Translocation t(2;3)(p15-23;q26-27) in myeloid malignancies: Report of 21 new cases clinical, cytogenetic and molecular genetic features

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