ETV6 rearrangements are recurrent in myeloid malignancies and are frequently associated with other genetic events.

Claudia Haferlach; Ulrike Bacher; Susanne Schnittger; Tamara Alpermann; Melanie Zenger; Wolfgang Kern; Torsten Haferlach

ETV6 rearrangements are recurrent in myeloid malignancies and are frequently associated with other genetic events.

Standard

ETV6 rearrangements are recurrent in myeloid malignancies and are frequently associated with other genetic events. / Haferlach, Claudia; Bacher, Ulrike; Schnittger, Susanne; Alpermann, Tamara; Zenger, Melanie; Kern, Wolfgang; Haferlach, Torsten.

in: GENE CHROMOSOME CANC, Jahrgang 51, Nr. 4, 4, 2012, S. 328-337.

Publikationen: SCORING: Beitrag in Fachzeitschrift/Zeitung › SCORING: Zeitschriftenaufsatz › Forschung › Begutachtung

Harvard

Haferlach, C, Bacher, U, Schnittger, S, Alpermann, T, Zenger, M, Kern, W & Haferlach, T 2012, 'ETV6 rearrangements are recurrent in myeloid malignancies and are frequently associated with other genetic events.', GENE CHROMOSOME CANC, Jg. 51, Nr. 4, 4, S. 328-337. <http://www.ncbi.nlm.nih.gov/pubmed/22162288?dopt=Citation>

APA

Haferlach, C., Bacher, U., Schnittger, S., Alpermann, T., Zenger, M., Kern, W., & Haferlach, T. (2012). ETV6 rearrangements are recurrent in myeloid malignancies and are frequently associated with other genetic events. GENE CHROMOSOME CANC, 51(4), 328-337. [4]. http://www.ncbi.nlm.nih.gov/pubmed/22162288?dopt=Citation

Vancouver

Haferlach C, Bacher U, Schnittger S, Alpermann T, Zenger M, Kern W et al. ETV6 rearrangements are recurrent in myeloid malignancies and are frequently associated with other genetic events. GENE CHROMOSOME CANC. 2012;51(4):328-337. 4.

Bibtex

@article{a567ea3d89ab4415a02e8a223a7e0eda,

title = "ETV6 rearrangements are recurrent in myeloid malignancies and are frequently associated with other genetic events.",

abstract = "ETV6 (TEL) rearrangements are favorable in pediatric acute lymphoblastic leukemia but are less well characterized in myeloid malignancies. We investigated 9,550 patients with myeloid disorders for ETV6 rearrangements by chromosome banding analysis and interphase fluorescence in situ hybridization. ETV6 rearrangements were identified in 51 of 9,550 (0.5%) patients (range, 19.2-85.3 years). Frequencies were in detail: acute myeloid leukemia (AML): 40 of 3,798, 1.1%; myelodysplastic syndromes (MDS): 6 of 3,375, 0.2%; myeloproliferative neoplasms (MPNs): 5 of 1,720, 0.3%; MDS/MPN: 0 of 210; and chronic myelomonocytic leukemia: 0 of 447. Thirty-three different partner bands of ETV6 were identified, and most were recurrent: 3q26 (n = 10), 5q33 (n = 4), 17q11 (n = 3), 22q12 (n = 3), 5q31 (n = 2), and 2q31 (n = 2). Additional chromosomal abnormalities were identified in 29 of 51 (57%) ETV6 rearranged cases. In AML, ETV6 rearrangements were frequently associated with NPM1 (9/39, 23%) and RUNX1 mutations (6/31, 19%). The FAB M0 subtype was more frequent in ETV6 rearranged de novo AML than other AML (P < 0.001); expression of CD7 and CD34 by immunophenotyping was higher in ETV6 rearranged AML compared with other subgroups. Survival of 29 ETV6 rearranged de novo AML was compared with 818 AML from other cytogenetic subgroups. Median overall and event-free survival of ETV6 rearranged cases was similar to the intermediate-risk cohort (26.3 vs. 62.2 months and 14.0 vs. 15.4 months) defined according to Medical Research Council criteria. Our study confirms the variety of ETV6 rearrangements in AML, MDS, and MPNs often in association with other genetic events. Prognosis of ETV6 rearranged de novo AML seems to be intermediate, which should be independently confirmed.",

author = "Claudia Haferlach and Ulrike Bacher and Susanne Schnittger and Tamara Alpermann and Melanie Zenger and Wolfgang Kern and Torsten Haferlach",

year = "2012",

language = "English",

volume = "51",

pages = "328--337",

journal = "GENE CHROMOSOME CANC",

issn = "1045-2257",

publisher = "Wiley-Liss Inc.",

number = "4",

}

RIS

TY - JOUR

T1 - ETV6 rearrangements are recurrent in myeloid malignancies and are frequently associated with other genetic events.

AU - Haferlach, Claudia

AU - Bacher, Ulrike

AU - Schnittger, Susanne

AU - Alpermann, Tamara

AU - Zenger, Melanie

AU - Kern, Wolfgang

AU - Haferlach, Torsten

PY - 2012

Y1 - 2012

N2 - ETV6 (TEL) rearrangements are favorable in pediatric acute lymphoblastic leukemia but are less well characterized in myeloid malignancies. We investigated 9,550 patients with myeloid disorders for ETV6 rearrangements by chromosome banding analysis and interphase fluorescence in situ hybridization. ETV6 rearrangements were identified in 51 of 9,550 (0.5%) patients (range, 19.2-85.3 years). Frequencies were in detail: acute myeloid leukemia (AML): 40 of 3,798, 1.1%; myelodysplastic syndromes (MDS): 6 of 3,375, 0.2%; myeloproliferative neoplasms (MPNs): 5 of 1,720, 0.3%; MDS/MPN: 0 of 210; and chronic myelomonocytic leukemia: 0 of 447. Thirty-three different partner bands of ETV6 were identified, and most were recurrent: 3q26 (n = 10), 5q33 (n = 4), 17q11 (n = 3), 22q12 (n = 3), 5q31 (n = 2), and 2q31 (n = 2). Additional chromosomal abnormalities were identified in 29 of 51 (57%) ETV6 rearranged cases. In AML, ETV6 rearrangements were frequently associated with NPM1 (9/39, 23%) and RUNX1 mutations (6/31, 19%). The FAB M0 subtype was more frequent in ETV6 rearranged de novo AML than other AML (P < 0.001); expression of CD7 and CD34 by immunophenotyping was higher in ETV6 rearranged AML compared with other subgroups. Survival of 29 ETV6 rearranged de novo AML was compared with 818 AML from other cytogenetic subgroups. Median overall and event-free survival of ETV6 rearranged cases was similar to the intermediate-risk cohort (26.3 vs. 62.2 months and 14.0 vs. 15.4 months) defined according to Medical Research Council criteria. Our study confirms the variety of ETV6 rearrangements in AML, MDS, and MPNs often in association with other genetic events. Prognosis of ETV6 rearranged de novo AML seems to be intermediate, which should be independently confirmed.

AB - ETV6 (TEL) rearrangements are favorable in pediatric acute lymphoblastic leukemia but are less well characterized in myeloid malignancies. We investigated 9,550 patients with myeloid disorders for ETV6 rearrangements by chromosome banding analysis and interphase fluorescence in situ hybridization. ETV6 rearrangements were identified in 51 of 9,550 (0.5%) patients (range, 19.2-85.3 years). Frequencies were in detail: acute myeloid leukemia (AML): 40 of 3,798, 1.1%; myelodysplastic syndromes (MDS): 6 of 3,375, 0.2%; myeloproliferative neoplasms (MPNs): 5 of 1,720, 0.3%; MDS/MPN: 0 of 210; and chronic myelomonocytic leukemia: 0 of 447. Thirty-three different partner bands of ETV6 were identified, and most were recurrent: 3q26 (n = 10), 5q33 (n = 4), 17q11 (n = 3), 22q12 (n = 3), 5q31 (n = 2), and 2q31 (n = 2). Additional chromosomal abnormalities were identified in 29 of 51 (57%) ETV6 rearranged cases. In AML, ETV6 rearrangements were frequently associated with NPM1 (9/39, 23%) and RUNX1 mutations (6/31, 19%). The FAB M0 subtype was more frequent in ETV6 rearranged de novo AML than other AML (P < 0.001); expression of CD7 and CD34 by immunophenotyping was higher in ETV6 rearranged AML compared with other subgroups. Survival of 29 ETV6 rearranged de novo AML was compared with 818 AML from other cytogenetic subgroups. Median overall and event-free survival of ETV6 rearranged cases was similar to the intermediate-risk cohort (26.3 vs. 62.2 months and 14.0 vs. 15.4 months) defined according to Medical Research Council criteria. Our study confirms the variety of ETV6 rearrangements in AML, MDS, and MPNs often in association with other genetic events. Prognosis of ETV6 rearranged de novo AML seems to be intermediate, which should be independently confirmed.

M3 - SCORING: Journal article

VL - 51

SP - 328

EP - 337

JO - GENE CHROMOSOME CANC

JF - GENE CHROMOSOME CANC

SN - 1045-2257

IS - 4

M1 - 4

ER -