Identification of a novel imatinib responsive KIF5B-PDGFRA fusion gene following screening for PDGFRA overexpression in patients with hypereosinophilia
Identification of a novel imatinib responsive KIF5B-PDGFRA fusion gene following screening for PDGFRA overexpression in patients with hypereosinophilia
Idiopathic hypereosinophilic syndrome (IHES) is a disease that is difficult to classify, and diagnosis is one of exclusion. The identification of a cytogenetically invisible interstitial deletion resulting in the fusion of FIP1-Like-1 (FIP1L1) to platelet-derived growth factor receptor alpha (PDGFRA) has enabled many IHES cases to be reclassified as chronic eosinophilic leukemia. As it is likely that PDGFRA may fuse to other partner genes, we established a reverse transcriptase-PCR test to detect specific overexpression of the PDGFRA kinase domain as an indicator of the presence of a fusion gene. Overexpression was detected in 12/12 FIP1L1-PDGFRA-positive patients, plus 9/217 (4%) patients with hypereosinophilia who had tested negative for FIP1L1-PDGFRA. One of the positive cases was investigated in detail and found to have a complex karyotype involving chromosomes 3, 4 and 10. Amplification of the genomic breakpoint by bubble PCR revealed a novel fusion between KIF5B at 10p11 and PDGFRA at 4q12. Imatinib, a known inhibitor of PDGFRalpha, produced a complete cytogenetic response and disappearance of the KIF5B-PDGFRA fusion by PCR, from both genomic DNA and mRNA. This study demonstrates the utility of screening for PDGFRA kinase domain overexpression in patients with IHES and has identified a third PDGFRA fusion partner in chronic myeloproliferative disorders.
chronic eosinophilic leukemia, imatinib, PDGFRA, KIF5B
827-832
Score, J.
939cd132-f752-4f83-8def-55d2aed25a46
Curtis, C.
e86c8e4e-9d89-4381-866d-df48af5bf8be
Waghorn, K.
60a6a26d-556b-41fc-84ee-dab95d63ab68
Stalder, M.
db3cea01-94a7-4bcc-af06-d1d1e98a2202
Jotterand, M.
eac30701-bf75-411e-bb31-ebfe4b2ce581
Grand, F.H.
f4b9e5f4-28c4-44d2-9916-d852c2fdaef8
Cross, N.C.
f87650da-b908-4a34-b31b-d62c5f186fe4
2006
Score, J.
939cd132-f752-4f83-8def-55d2aed25a46
Curtis, C.
e86c8e4e-9d89-4381-866d-df48af5bf8be
Waghorn, K.
60a6a26d-556b-41fc-84ee-dab95d63ab68
Stalder, M.
db3cea01-94a7-4bcc-af06-d1d1e98a2202
Jotterand, M.
eac30701-bf75-411e-bb31-ebfe4b2ce581
Grand, F.H.
f4b9e5f4-28c4-44d2-9916-d852c2fdaef8
Cross, N.C.
f87650da-b908-4a34-b31b-d62c5f186fe4
Score, J., Curtis, C., Waghorn, K., Stalder, M., Jotterand, M., Grand, F.H. and Cross, N.C.
(2006)
Identification of a novel imatinib responsive KIF5B-PDGFRA fusion gene following screening for PDGFRA overexpression in patients with hypereosinophilia.
Leukemia, 20 (5), .
(doi:10.1038/sj.leu.2404154).
Abstract
Idiopathic hypereosinophilic syndrome (IHES) is a disease that is difficult to classify, and diagnosis is one of exclusion. The identification of a cytogenetically invisible interstitial deletion resulting in the fusion of FIP1-Like-1 (FIP1L1) to platelet-derived growth factor receptor alpha (PDGFRA) has enabled many IHES cases to be reclassified as chronic eosinophilic leukemia. As it is likely that PDGFRA may fuse to other partner genes, we established a reverse transcriptase-PCR test to detect specific overexpression of the PDGFRA kinase domain as an indicator of the presence of a fusion gene. Overexpression was detected in 12/12 FIP1L1-PDGFRA-positive patients, plus 9/217 (4%) patients with hypereosinophilia who had tested negative for FIP1L1-PDGFRA. One of the positive cases was investigated in detail and found to have a complex karyotype involving chromosomes 3, 4 and 10. Amplification of the genomic breakpoint by bubble PCR revealed a novel fusion between KIF5B at 10p11 and PDGFRA at 4q12. Imatinib, a known inhibitor of PDGFRalpha, produced a complete cytogenetic response and disappearance of the KIF5B-PDGFRA fusion by PCR, from both genomic DNA and mRNA. This study demonstrates the utility of screening for PDGFRA kinase domain overexpression in patients with IHES and has identified a third PDGFRA fusion partner in chronic myeloproliferative disorders.
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Published date: 2006
Keywords:
chronic eosinophilic leukemia, imatinib, PDGFRA, KIF5B
Identifiers
Local EPrints ID: 40672
URI: http://eprints.soton.ac.uk/id/eprint/40672
ISSN: 0887-6924
PURE UUID: b521e4bd-522a-4df6-9d54-8e8b936810dc
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Date deposited: 07 Jul 2006
Last modified: 16 Mar 2024 03:23
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Contributors
Author:
J. Score
Author:
C. Curtis
Author:
K. Waghorn
Author:
M. Stalder
Author:
M. Jotterand
Author:
F.H. Grand
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