EVI1 overexpression in distinct subtypes of pediatric acute myeloid leukemia

B. V. Balgobind; S. Lugthart; I. H. Hollink; S. T.J.C.M. Arentsen-Peters; E. R. Van Wering; S. S.N. De Graaf; D. Reinhardt; U. Creutzig; G. J.L. Kaspers; E. S.J.M. De Bont; J. Stary; J. Trka; M. Zimmermann; H. B. Beverloo; R. Pieters; R. Delwel; C. M. Zwaan; M. M. Van Den Heuvel-Eibrink

doi:10.1038/leu.2010.47

EVI1 overexpression in distinct subtypes of pediatric acute myeloid leukemia

B. V. Balgobind, S. Lugthart, I. H. Hollink, S. T.J.C.M. Arentsen-Peters, E. R. Van Wering, S. S.N. De Graaf, D. Reinhardt, U. Creutzig, G. J.L. Kaspers, E. S.J.M. De Bont, J. Stary, J. Trka, M. Zimmermann, H. B. Beverloo, R. Pieters, R. Delwel, C. M. Zwaan, M. M. Van Den Heuvel-Eibrink

Onderzoeksoutput: Bijdrage aan tijdschrift › Artikel › peer review

72 Citaten (Scopus)

Samenvatting

Overexpression of the ecotropic virus integration-1 (EVI1+) gene (EVI1), localized at chromosome 3q26, is associated with adverse outcome in adult acute myeloid leukemia (AML). In pediatric AML, 3q26 abnormalities are rare, and the role of EVI1 is unknown. We studied 228 pediatric AML samples for EVI1 using gene expression profiling and RQ-PCR. EVI1 was found in 20/213 (9%) of children with de novo AML, and in 4/8 with secondary AML. It was predominantly found in MLL-rearranged AML (13/47), monosomy 7 (2/3), or FAB M6/7 (6/10), and mutually exclusive with core-binding factor AML, t(15;17), and NPM1 mutations. Fluorescent in situ hybridization (FISH) was performed to detect cryptic 3q26 abnormalities. However, none of the EVI1+ patients harbored structural 3q26 alterations. Although significant differences in 4 years pEFS for EVI1+ and EVI1-pediatric AML were observed (28% ±11 vs 44%±4, P=0.04), multivariate analysis did not identify EVI1 as an independent prognostic factor. We conclude that EVI1+ can be found in ∼10% of pediatric AML. Although EVI1+ was not an independent prognostic factor, it was predominantly found in subtypes of pediatric AML that are related with an intermediate to unfavorable prognosis. Further research should explain the role of EVI1+ in disease biology in these cases. Remarkably, no 3q26 abnormalities were identified in EVI1+ pediatric AML.

Originele taal-2	Engels
Pagina's (van-tot)	942-949
Aantal pagina's	8
Tijdschrift	Leukemia
Volume	24
Nummer van het tijdschrift	5
DOI's	https://doi.org/10.1038/leu.2010.47
Status	Gepubliceerd - mei 2010
Extern gepubliceerd	Ja

Toegang tot document

10.1038/leu.2010.47

Citeer dit

Balgobind, B. V., Lugthart, S., Hollink, I. H., Arentsen-Peters, S. T. J. C. M., Van Wering, E. R., De Graaf, S. S. N., Reinhardt, D., Creutzig, U., Kaspers, G. J. L., De Bont, E. S. J. M., Stary, J., Trka, J., Zimmermann, M., Beverloo, H. B., Pieters, R., Delwel, R., Zwaan, C. M., & Van Den Heuvel-Eibrink, M. M. (2010). EVI1 overexpression in distinct subtypes of pediatric acute myeloid leukemia. Leukemia, 24(5), 942-949. https://doi.org/10.1038/leu.2010.47

@article{0ed08802d654457fbc3b7e22cdb7d4e2,

title = "EVI1 overexpression in distinct subtypes of pediatric acute myeloid leukemia",

abstract = "Overexpression of the ecotropic virus integration-1 (EVI1+) gene (EVI1), localized at chromosome 3q26, is associated with adverse outcome in adult acute myeloid leukemia (AML). In pediatric AML, 3q26 abnormalities are rare, and the role of EVI1 is unknown. We studied 228 pediatric AML samples for EVI1 using gene expression profiling and RQ-PCR. EVI1 was found in 20/213 (9%) of children with de novo AML, and in 4/8 with secondary AML. It was predominantly found in MLL-rearranged AML (13/47), monosomy 7 (2/3), or FAB M6/7 (6/10), and mutually exclusive with core-binding factor AML, t(15;17), and NPM1 mutations. Fluorescent in situ hybridization (FISH) was performed to detect cryptic 3q26 abnormalities. However, none of the EVI1+ patients harbored structural 3q26 alterations. Although significant differences in 4 years pEFS for EVI1+ and EVI1-pediatric AML were observed (28% ±11 vs 44%±4, P=0.04), multivariate analysis did not identify EVI1 as an independent prognostic factor. We conclude that EVI1+ can be found in ∼10% of pediatric AML. Although EVI1+ was not an independent prognostic factor, it was predominantly found in subtypes of pediatric AML that are related with an intermediate to unfavorable prognosis. Further research should explain the role of EVI1+ in disease biology in these cases. Remarkably, no 3q26 abnormalities were identified in EVI1+ pediatric AML.",

keywords = "EVI1 expression, MDS1/EVI1 expression, Pediatric AML",

author = "Balgobind, {B. V.} and S. Lugthart and Hollink, {I. H.} and Arentsen-Peters, {S. T.J.C.M.} and {Van Wering}, {E. R.} and {De Graaf}, {S. S.N.} and D. Reinhardt and U. Creutzig and Kaspers, {G. J.L.} and {De Bont}, {E. S.J.M.} and J. Stary and J. Trka and M. Zimmermann and Beverloo, {H. B.} and R. Pieters and R. Delwel and Zwaan, {C. M.} and {Van Den Heuvel-Eibrink}, {M. M.}",

note = "Funding Information: This work was funded by the NWO {\textquoteleft}Netherlands Organization for Scientific Research{\textquoteright} (BVB), KOCR {\textquoteleft}Kinder-Oncologisch Centrum Rotterdam{\textquoteright} (BVB and IHH) and EHA (SL).",

year = "2010",

month = may,

doi = "10.1038/leu.2010.47",

language = "English",

volume = "24",

pages = "942--949",

journal = "Leukemia",

issn = "0887-6924",

publisher = "Springer Nature",

number = "5",

}

Balgobind, BV, Lugthart, S, Hollink, IH, Arentsen-Peters, STJCM, Van Wering, ER, De Graaf, SSN, Reinhardt, D, Creutzig, U, Kaspers, GJL, De Bont, ESJM, Stary, J, Trka, J, Zimmermann, M, Beverloo, HB, Pieters, R, Delwel, R, Zwaan, CM & Van Den Heuvel-Eibrink, MM 2010, 'EVI1 overexpression in distinct subtypes of pediatric acute myeloid leukemia', Leukemia, vol. 24, nr. 5, blz. 942-949. https://doi.org/10.1038/leu.2010.47

TY - JOUR

T1 - EVI1 overexpression in distinct subtypes of pediatric acute myeloid leukemia

AU - Balgobind, B. V.

AU - Lugthart, S.

AU - Hollink, I. H.

AU - Arentsen-Peters, S. T.J.C.M.

AU - Van Wering, E. R.

AU - De Graaf, S. S.N.

AU - Reinhardt, D.

AU - Creutzig, U.

AU - Kaspers, G. J.L.

AU - De Bont, E. S.J.M.

AU - Stary, J.

AU - Trka, J.

AU - Zimmermann, M.

AU - Beverloo, H. B.

AU - Pieters, R.

AU - Delwel, R.

AU - Zwaan, C. M.

AU - Van Den Heuvel-Eibrink, M. M.

N1 - Funding Information: This work was funded by the NWO ‘Netherlands Organization for Scientific Research’ (BVB), KOCR ‘Kinder-Oncologisch Centrum Rotterdam’ (BVB and IHH) and EHA (SL).

PY - 2010/5

Y1 - 2010/5

N2 - Overexpression of the ecotropic virus integration-1 (EVI1+) gene (EVI1), localized at chromosome 3q26, is associated with adverse outcome in adult acute myeloid leukemia (AML). In pediatric AML, 3q26 abnormalities are rare, and the role of EVI1 is unknown. We studied 228 pediatric AML samples for EVI1 using gene expression profiling and RQ-PCR. EVI1 was found in 20/213 (9%) of children with de novo AML, and in 4/8 with secondary AML. It was predominantly found in MLL-rearranged AML (13/47), monosomy 7 (2/3), or FAB M6/7 (6/10), and mutually exclusive with core-binding factor AML, t(15;17), and NPM1 mutations. Fluorescent in situ hybridization (FISH) was performed to detect cryptic 3q26 abnormalities. However, none of the EVI1+ patients harbored structural 3q26 alterations. Although significant differences in 4 years pEFS for EVI1+ and EVI1-pediatric AML were observed (28% ±11 vs 44%±4, P=0.04), multivariate analysis did not identify EVI1 as an independent prognostic factor. We conclude that EVI1+ can be found in ∼10% of pediatric AML. Although EVI1+ was not an independent prognostic factor, it was predominantly found in subtypes of pediatric AML that are related with an intermediate to unfavorable prognosis. Further research should explain the role of EVI1+ in disease biology in these cases. Remarkably, no 3q26 abnormalities were identified in EVI1+ pediatric AML.

AB - Overexpression of the ecotropic virus integration-1 (EVI1+) gene (EVI1), localized at chromosome 3q26, is associated with adverse outcome in adult acute myeloid leukemia (AML). In pediatric AML, 3q26 abnormalities are rare, and the role of EVI1 is unknown. We studied 228 pediatric AML samples for EVI1 using gene expression profiling and RQ-PCR. EVI1 was found in 20/213 (9%) of children with de novo AML, and in 4/8 with secondary AML. It was predominantly found in MLL-rearranged AML (13/47), monosomy 7 (2/3), or FAB M6/7 (6/10), and mutually exclusive with core-binding factor AML, t(15;17), and NPM1 mutations. Fluorescent in situ hybridization (FISH) was performed to detect cryptic 3q26 abnormalities. However, none of the EVI1+ patients harbored structural 3q26 alterations. Although significant differences in 4 years pEFS for EVI1+ and EVI1-pediatric AML were observed (28% ±11 vs 44%±4, P=0.04), multivariate analysis did not identify EVI1 as an independent prognostic factor. We conclude that EVI1+ can be found in ∼10% of pediatric AML. Although EVI1+ was not an independent prognostic factor, it was predominantly found in subtypes of pediatric AML that are related with an intermediate to unfavorable prognosis. Further research should explain the role of EVI1+ in disease biology in these cases. Remarkably, no 3q26 abnormalities were identified in EVI1+ pediatric AML.

KW - EVI1 expression

KW - MDS1/EVI1 expression

KW - Pediatric AML

UR - http://www.scopus.com/inward/record.url?scp=77952426083&partnerID=8YFLogxK

U2 - 10.1038/leu.2010.47

DO - 10.1038/leu.2010.47

M3 - Article

AN - SCOPUS:77952426083

SN - 0887-6924

VL - 24

SP - 942

EP - 949

JO - Leukemia

JF - Leukemia

IS - 5

ER -

EVI1 overexpression in distinct subtypes of pediatric acute myeloid leukemia

Samenvatting

Toegang tot document

Vingerafdruk

Citeer dit