FLT3 and KIT mutated pediatric acute myeloid leukemia (AML) samples are sensitive in vitro to the tyrosine kinase inhibitor SU11657

Bianca F. Goemans; Christian M. Zwaan; Jacqueline Cloos; Desiree de Lange; Anne H. Loonen; Dirk Reinhardt; Karel Hählen; Brenda E.S. Gibson; Ursula Creutzig; Gertjan J.L. Kaspers

doi:10.1016/j.leukres.2010.04.004

FLT3 and KIT mutated pediatric acute myeloid leukemia (AML) samples are sensitive in vitro to the tyrosine kinase inhibitor SU11657

Bianca F. Goemans
, Christian M. Zwaan
, Jacqueline Cloos
, Desiree de Lange
, Anne H. Loonen
, Dirk Reinhardt
, Karel Hählen
, Brenda E.S. Gibson
, Ursula Creutzig
, Gertjan J.L. Kaspers

Research output: Contribution to journal › Article › peer-review

7 Citations (Scopus)

Abstract

New treatment strategies to improve the outcome of pediatric acute myeloid leukemia (AML) are required as 40% of children diagnosed with AML do not survive. Around 30% of pediatric AML patients harbour a mutation in the tyrosine kinases FLT3 (±20%) or KIT (±10%). In this study we investigated whether pediatric AML samples (N= 61) were sensitive to the tyrosine kinase inhibitor SU11657 (similar to the clinically available drug sunitinib) in vitro, and whether sensitivity was related to expression of, and mutations in, FLT3 and KIT. Overall, SU11657 showed only moderate cytotoxicity. A FLT3 mutation was detected in 35% and a KIT mutation in 8% of the samples. FLT3 and KIT mutated samples were significantly more sensitive to SU11657 than WT KIT and FLT3 samples. Samples without KIT or FLT3 mutations, but with a high wild-type (WT) KIT expression were significantly more sensitive to SU11657 than samples with low KIT expression. Further clinical evaluation of SU11657 and sunitinib combined with chemotherapy would be of interest. Inclusion in clinical trials should not be restricted to patients with FLT3 or KIT mutations.

Original language	English
Pages (from-to)	1302-1307
Number of pages	6
Journal	Leukemia Research
Volume	34
Issue number	10
DOIs	https://doi.org/10.1016/j.leukres.2010.04.004
Publication status	Published - Oct 2010
Externally published	Yes

Keywords

Acute myeloid leukemia
Childhood leukemia
Drug sensitivity
Flt3
Tyrosine kinase inhibitor

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10.1016/j.leukres.2010.04.004

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Goemans, B. F., Zwaan, C. M., Cloos, J., de Lange, D., Loonen, A. H., Reinhardt, D., Hählen, K., Gibson, B. E. S., Creutzig, U., & Kaspers, G. J. L. (2010). FLT3 and KIT mutated pediatric acute myeloid leukemia (AML) samples are sensitive in vitro to the tyrosine kinase inhibitor SU11657. Leukemia Research, 34(10), 1302-1307. https://doi.org/10.1016/j.leukres.2010.04.004

@article{30c88b4258cb4699ac908a4fa45ce7cd,

title = "FLT3 and KIT mutated pediatric acute myeloid leukemia (AML) samples are sensitive in vitro to the tyrosine kinase inhibitor SU11657",

abstract = "New treatment strategies to improve the outcome of pediatric acute myeloid leukemia (AML) are required as 40\% of children diagnosed with AML do not survive. Around 30\% of pediatric AML patients harbour a mutation in the tyrosine kinases FLT3 (±20\%) or KIT (±10\%). In this study we investigated whether pediatric AML samples (N= 61) were sensitive to the tyrosine kinase inhibitor SU11657 (similar to the clinically available drug sunitinib) in vitro, and whether sensitivity was related to expression of, and mutations in, FLT3 and KIT. Overall, SU11657 showed only moderate cytotoxicity. A FLT3 mutation was detected in 35\% and a KIT mutation in 8\% of the samples. FLT3 and KIT mutated samples were significantly more sensitive to SU11657 than WT KIT and FLT3 samples. Samples without KIT or FLT3 mutations, but with a high wild-type (WT) KIT expression were significantly more sensitive to SU11657 than samples with low KIT expression. Further clinical evaluation of SU11657 and sunitinib combined with chemotherapy would be of interest. Inclusion in clinical trials should not be restricted to patients with FLT3 or KIT mutations.",

keywords = "Acute myeloid leukemia, Childhood leukemia, Drug sensitivity, Flt3, Tyrosine kinase inhibitor",

author = "Goemans, \{Bianca F.\} and Zwaan, \{Christian M.\} and Jacqueline Cloos and \{de Lange\}, Desiree and Loonen, \{Anne H.\} and Dirk Reinhardt and Karel H{\"a}hlen and Gibson, \{Brenda E.S.\} and Ursula Creutzig and Kaspers, \{Gertjan J.L.\}",

note = "Funding Information: The authors wish to thank all the patients, as well as the hospitals and clinicians participating in the AML-BFM Study Group, the MRC Childhood Leukaemia Working Party and the Dutch Childhood Oncology Group, as well as their reference laboratories, who provided us with the patient samples and the clinical and cell-biological data. This work was performed in the setting of the International BFM Study Group (chaired by M. Schrappe, Kiel, Germany). The technicians of the research laboratory of Pediatric Oncology of the VU University Medical Center handled all samples. This work was partially funded by ZonMW AGIKO grant 920-03-374 (BFG). SU11657 was provided free of charge by Sugen Inc (now Pfizer Inc). ",

year = "2010",

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doi = "10.1016/j.leukres.2010.04.004",

language = "English",

volume = "34",

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journal = "Leukemia Research",

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T1 - FLT3 and KIT mutated pediatric acute myeloid leukemia (AML) samples are sensitive in vitro to the tyrosine kinase inhibitor SU11657

AU - Goemans, Bianca F.

AU - Zwaan, Christian M.

AU - Cloos, Jacqueline

AU - de Lange, Desiree

AU - Loonen, Anne H.

AU - Reinhardt, Dirk

AU - Hählen, Karel

AU - Gibson, Brenda E.S.

AU - Creutzig, Ursula

AU - Kaspers, Gertjan J.L.

N1 - Funding Information: The authors wish to thank all the patients, as well as the hospitals and clinicians participating in the AML-BFM Study Group, the MRC Childhood Leukaemia Working Party and the Dutch Childhood Oncology Group, as well as their reference laboratories, who provided us with the patient samples and the clinical and cell-biological data. This work was performed in the setting of the International BFM Study Group (chaired by M. Schrappe, Kiel, Germany). The technicians of the research laboratory of Pediatric Oncology of the VU University Medical Center handled all samples. This work was partially funded by ZonMW AGIKO grant 920-03-374 (BFG). SU11657 was provided free of charge by Sugen Inc (now Pfizer Inc).

PY - 2010/10

Y1 - 2010/10

N2 - New treatment strategies to improve the outcome of pediatric acute myeloid leukemia (AML) are required as 40% of children diagnosed with AML do not survive. Around 30% of pediatric AML patients harbour a mutation in the tyrosine kinases FLT3 (±20%) or KIT (±10%). In this study we investigated whether pediatric AML samples (N= 61) were sensitive to the tyrosine kinase inhibitor SU11657 (similar to the clinically available drug sunitinib) in vitro, and whether sensitivity was related to expression of, and mutations in, FLT3 and KIT. Overall, SU11657 showed only moderate cytotoxicity. A FLT3 mutation was detected in 35% and a KIT mutation in 8% of the samples. FLT3 and KIT mutated samples were significantly more sensitive to SU11657 than WT KIT and FLT3 samples. Samples without KIT or FLT3 mutations, but with a high wild-type (WT) KIT expression were significantly more sensitive to SU11657 than samples with low KIT expression. Further clinical evaluation of SU11657 and sunitinib combined with chemotherapy would be of interest. Inclusion in clinical trials should not be restricted to patients with FLT3 or KIT mutations.

AB - New treatment strategies to improve the outcome of pediatric acute myeloid leukemia (AML) are required as 40% of children diagnosed with AML do not survive. Around 30% of pediatric AML patients harbour a mutation in the tyrosine kinases FLT3 (±20%) or KIT (±10%). In this study we investigated whether pediatric AML samples (N= 61) were sensitive to the tyrosine kinase inhibitor SU11657 (similar to the clinically available drug sunitinib) in vitro, and whether sensitivity was related to expression of, and mutations in, FLT3 and KIT. Overall, SU11657 showed only moderate cytotoxicity. A FLT3 mutation was detected in 35% and a KIT mutation in 8% of the samples. FLT3 and KIT mutated samples were significantly more sensitive to SU11657 than WT KIT and FLT3 samples. Samples without KIT or FLT3 mutations, but with a high wild-type (WT) KIT expression were significantly more sensitive to SU11657 than samples with low KIT expression. Further clinical evaluation of SU11657 and sunitinib combined with chemotherapy would be of interest. Inclusion in clinical trials should not be restricted to patients with FLT3 or KIT mutations.

KW - Acute myeloid leukemia

KW - Childhood leukemia

KW - Drug sensitivity

KW - Flt3

KW - Tyrosine kinase inhibitor

UR - https://www.scopus.com/pages/publications/77955980691

U2 - 10.1016/j.leukres.2010.04.004

DO - 10.1016/j.leukres.2010.04.004

M3 - Article

C2 - 20435347

AN - SCOPUS:77955980691

SN - 0145-2126

VL - 34

SP - 1302

EP - 1307

JO - Leukemia Research

JF - Leukemia Research

IS - 10

ER -

FLT3 and KIT mutated pediatric acute myeloid leukemia (AML) samples are sensitive in vitro to the tyrosine kinase inhibitor SU11657

Abstract

Keywords

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