TY - JOUR
T1 - Clinical relevance of Wilms tumor 1 gene mutations in childhood acute myeloid leukemia
AU - Hollink, Iris H.I.M.
AU - Van Den Heuvel-Eibrink, Marry M.
AU - Zimmermann, Martin
AU - Balgobind, Brian V.
AU - Arentsen-Peters, Susan T.C.J.M.
AU - Alders, Marielle
AU - Willasch, Andre
AU - Kaspers, Gertjan J.L.
AU - Trka, Jan
AU - Baruchel, Andre
AU - De Graaf, Siebold S.N.
AU - Creutzig, Ursula
AU - Pieters, Rob
AU - Reinhardt, Dirk
AU - Zwaan, C. Michel
PY - 2009
Y1 - 2009
N2 - Wilms tumor 1 (WT1) mutations have recently been identified in approximately 10% of adult acute myeloid leukemia (AML) with normal cytogenetics (CN-AML) and are associated with poor outcome. Using array-based comparative genome hybridization in pediatric CN-AML samples, we detected a WT1 deletion in one sample. The other WT1 allele was mutated. This prompted us to further investigate the role of WT1 aberrations in childhood AML. Mutations were found in 35 of 298 (12%) diagnostic pediatric AML samples. In 19 of 35 (54%) samples, more than one WT1 aberration was found: 15 samples had 2 different mutations, 2 had a homozygous mutation, and 2 had a mutation plus a WT1 deletion. WT1 mutations clustered significantly in the CN-AML subgroup (22%; P < .001) and were associated with FLT3/ITD (43 vs 17%; P < .001). WT1 mutations conferred an independent poor prognostic significance (WT1 mutated vs wild-type patients: 5-year probability of overall survival [pOS] 35% vs 66%, P = .002; probability of event-free survival 22% vs 46%, P < .001; and cumulative incidence of relapse or regression 70% vs 44%, P < .001). Patients with both a WT1 mutation and a FLT3/ITD had a dismal prognosis (5-year pOS 21%). WT1 mutations occur at a significant rate in childhood AML and are a novel independent poor prognostic marker.
AB - Wilms tumor 1 (WT1) mutations have recently been identified in approximately 10% of adult acute myeloid leukemia (AML) with normal cytogenetics (CN-AML) and are associated with poor outcome. Using array-based comparative genome hybridization in pediatric CN-AML samples, we detected a WT1 deletion in one sample. The other WT1 allele was mutated. This prompted us to further investigate the role of WT1 aberrations in childhood AML. Mutations were found in 35 of 298 (12%) diagnostic pediatric AML samples. In 19 of 35 (54%) samples, more than one WT1 aberration was found: 15 samples had 2 different mutations, 2 had a homozygous mutation, and 2 had a mutation plus a WT1 deletion. WT1 mutations clustered significantly in the CN-AML subgroup (22%; P < .001) and were associated with FLT3/ITD (43 vs 17%; P < .001). WT1 mutations conferred an independent poor prognostic significance (WT1 mutated vs wild-type patients: 5-year probability of overall survival [pOS] 35% vs 66%, P = .002; probability of event-free survival 22% vs 46%, P < .001; and cumulative incidence of relapse or regression 70% vs 44%, P < .001). Patients with both a WT1 mutation and a FLT3/ITD had a dismal prognosis (5-year pOS 21%). WT1 mutations occur at a significant rate in childhood AML and are a novel independent poor prognostic marker.
UR - http://www.scopus.com/inward/record.url?scp=67651096058&partnerID=8YFLogxK
U2 - 10.1182/blood-2008-09-177949
DO - 10.1182/blood-2008-09-177949
M3 - Article
C2 - 19171881
AN - SCOPUS:67651096058
SN - 0006-4971
VL - 113
SP - 5951
EP - 5960
JO - Blood
JF - Blood
IS - 23
ER -