Clinical Impact of Additional Cytogenetic Aberrations, cKIT and RAS Mutations, and Treatment Elements in Pediatric t(8;21)-AML: Results From an International Retrospective Study by the International Berlin-Frankfurt-Munster Study Group

被引:67
|
作者
Klein, Kim [1 ]
Kaspers, Gertjan [1 ,2 ]
Harrison, Christine J. [4 ]
Beverloo, H. Berna [3 ]
Reedijk, Ardine [2 ]
Bongers, Mathilda [1 ]
Cloos, Jacqueline [1 ]
Pession, Andrea [6 ]
Reinhardt, Dirk [7 ]
Zimmerman, Martin [8 ]
Creutzig, Ursula [8 ]
Dworzak, Michael [9 ]
Alonzo, Todd [10 ,11 ]
Johnston, Donna [10 ,11 ]
Hirsch, Betsy [10 ,11 ]
Zapotocky, Michal [12 ]
De Moerloose, Barbara [13 ]
Fynn, Alcira [14 ]
Lee, Vincent [15 ]
Taga, Takashi [16 ]
Tawa, Akio [17 ]
Auvrignon, Anne [18 ]
Zeller, Bernward [19 ]
Forestier, Erik [20 ]
Salgado, Carmen [21 ]
Balwierz, Walentyna [22 ]
Popa, Alexander [23 ]
Rubnitz, Jeffrey [24 ]
Raimondi, Susana [24 ]
Gibson, Brenda [5 ]
机构
[1] Vrije Univ Amsterdam, Med Ctr, NL-1081 HZ Amsterdam, Netherlands
[2] Dutch Childhood Oncol Grp, The Hague, Netherlands
[3] Erasmus MC, Rotterdam, Netherlands
[4] Newcastle Univ, Newcastle Upon Tyne NE1 7RU, Tyne & Wear, England
[5] Royal Hosp Sick Children, Glasgow G3 8SJ, Lanark, Scotland
[6] Italian Assoc Pediat Hematol Oncol, Bologna, Italy
[7] Berlin Frankfurt Munster BFM Germany, Essen, Germany
[8] BFM Germany, Hannover, Germany
[9] BFM Austria, Vienna, Austria
[10] Childrens Oncol Grp, Canc Grp, Philadelphia, PA USA
[11] Pediat Oncol Grp, Philadelphia, PA USA
[12] Czech Paediat Hematol Working Grp, Prague, Czech Republic
[13] European Org Res Treatment Canc, Childrens Leukemia Grp, Brussels, Belgium
[14] Grp Argentino Tratamiento Leucemia Aguda, Buenos Aires, DF, Argentina
[15] Hong Kong Paediat Haematol & Oncol Study Grp, Hong Kong, Hong Kong, Peoples R China
[16] Japanese Pediat Leukemia Lymphoma Study Grp, Otsu, Shiga, Japan
[17] Japanese Pediat Leukemia Lymphoma Study Grp, Osaka, Japan
[18] French Leucemie Aigue Myeloblast Enfant Cooperat, Paris, France
[19] Nord Soc Paediat Haematol & Oncol, Oslo, Norway
[20] Nord Soc Paediat Haematol & Oncol, Umea, Sweden
[21] Natl Program Antineoplast Drugs Children, Santiago, Chile
[22] Polish Pediat Leukemia Lymphoma Study Grp, Krakow, Poland
[23] Russian Acute Myeloid Leukemia Study Grp, Moscow, Russia
[24] St Jude Childrens Res Hosp, Memphis, TN 38105 USA
关键词
ACUTE MYELOID-LEUKEMIA; HIGH-DOSE CYTARABINE; COOPERATIVE-STUDY-GROUP; PROGNOSTIC-SIGNIFICANCE; ONCOLOGY-GROUP; CHROMOSOMAL-ABNORMALITIES; TANDEM DUPLICATION; KIT MUTATIONS; C-KIT; AML;
D O I
10.1200/JCO.2015.61.1947
中图分类号
R73 [肿瘤学];
学科分类号
100214 ;
摘要
Purpose This retrospective cohort study aimed to determine the predictive relevance of clinical characteristics, additional cytogenetic aberrations, and cKIT and RAS mutations, as well as to evaluate whether specific treatment elements were associated with outcomes in pediatric t(8;21)-positive patients with acute myeloid leukemia (AML). Patients and Methods Karyotypes of 916 pediatric patients with t(8;21)-AML were reviewed for the presence of additional cytogenetic aberrations, and 228 samples were screened for presence of cKIT and RAS mutations. Multivariable regression models were used to assess the relevance of anthracyclines, cytarabine, and etoposide during induction and overall treatment. End points were the probability of achieving complete remission, cumulative incidence of relapse (CIR), probability of event-free survival, and probability of overall survival. Results Of 838 patients included in final analyses, 92% achieved complete remission. The 5-year overall survival, event-free survival, and CIR were 74%, 58%, and 26%, respectively. cKIT mutations and RAS mutations were not significantly associated with outcome. Patients with deletions of chromosome arm 9q [del(9q); n = 104] had a lower probability of complete remission (P = .01). Gain of chromosome 4 (+4; n = 21) was associated with inferior CIR and survival (P < .01). Anthracycline doses greater than 150 mg/m(2) and etoposide doses greater than 500 mg/m(2) in the first induction course and high-dose cytarabine 3 g/m(2) during induction were associated with better outcomes on various end points. Cumulative doses of cytarabine greater than 30 g/m(2) and etoposide greater than 1,500 mg/m(2) were associated with lower CIR rates and better probability of event-free survival. Conclusion Pediatric patients with t(8;21)-AML and additional del(9q) or additional +4 might not be considered at good risk. Patients with t(8;21)-AML likely benefit from protocols that have high doses of anthracyclines, etoposide, and cytarabine during induction, as well as from protocols comprising cumulative high doses of cytarabine and etoposide. (C) 2015 by American Society of Clinical Oncology
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页码:4247 / 4258
页数:12
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