The molecular anatomy of the FIP1L1-PDGFRA fusion gene
The molecular anatomy of the FIP1L1-PDGFRA fusion gene
The FIP1L1-PDGFRA fusion gene is a recurrent molecular abnormality in patients with eosinophilia-associated myeloproliferative neoplasms. We characterized FIP1L1-PDGFRA junction sequences from 113 patients at the mRNA (n=113) and genomic DNA (n=85) levels. Transcript types could be assigned in 109 patients as type A (n=50, 46%) or B (n=47, 43%), which were created by cryptic acceptor splice sites in different introns of FIP1L1 (type A) or within PDGFRA exon 12 (type B). We also characterized a new transcript type C (n=12, 11%) in which both genomic breakpoints fell within coding sequences creating a hybrid exon without use of a cryptic acceptor splice site. The location of genomic breakpoints within PDGFRA and the availability of AG splice sites determine the transcript type and restrict the FIP1L1 exons used for the creation of the fusion. Stretches of overlapping sequences were identified at the genomic junction site, suggesting that the FIP1L1-PDGFRA fusion is created by illegitimate non-homologous end-joining. Statistical analyses provided evidence for clustering of breakpoints within FIP1L1 that may be related to DNA- or chromatin-related structural features. The variability in the anatomy of the FIP1L1-PDGFRA fusion has important implications for strategies to detect the fusion at diagnosis or for monitoring response to treatment
FIP1L1, PDGFRA, Eos-MPN
271-278
Walz, C.
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Score, J.
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Mix, J.
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Cilloni, D.
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Roche-Lestienne, C.
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Yeh, R.F.
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Wiemels, J.L.
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Ottaviani, E.
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Erben, P.
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Hochhaus, A.
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Baccarani, M.
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Grimwade, D.
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Preudhomme, C.
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Apperley, J.
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Martinelli, G.
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Saglio, G.
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Cross, N.C.
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Reiter, A.
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February 2009
Walz, C.
03a7b61b-bebd-4510-8f08-ec6b65a36809
Score, J.
ea0db6ef-c17e-4915-b216-ac67c07b26b7
Mix, J.
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Cilloni, D.
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Roche-Lestienne, C.
b14a6275-0a49-450d-9d0a-0750986d2060
Yeh, R.F.
96f8be17-4226-4982-b53a-3a2d3334da13
Wiemels, J.L.
334b0452-86c3-45ae-9452-3af1388ea7f5
Ottaviani, E.
76295991-0c99-42c8-8170-52db831a6ef1
Erben, P.
50e7cc94-7147-4f08-9a95-86b4aade442c
Hochhaus, A.
4c0b9da4-adfa-4253-8af7-78cec9e9a24f
Baccarani, M.
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Grimwade, D.
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Preudhomme, C.
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Apperley, J.
622c945c-74c1-4773-a80f-2bdafe8dfe14
Martinelli, G.
3949da7a-7efe-4ebd-b1f7-92f1ca150d66
Saglio, G.
73d6fc31-81e4-4e8d-9ea3-e08db4d00f10
Cross, N.C.
f87650da-b908-4a34-b31b-d62c5f186fe4
Reiter, A.
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Walz, C., Score, J., Mix, J., Cilloni, D., Roche-Lestienne, C., Yeh, R.F., Wiemels, J.L., Ottaviani, E., Erben, P., Hochhaus, A., Baccarani, M., Grimwade, D., Preudhomme, C., Apperley, J., Martinelli, G., Saglio, G., Cross, N.C. and Reiter, A.
(2009)
The molecular anatomy of the FIP1L1-PDGFRA fusion gene.
Leukemia, 23 (2), .
(doi:10.1038/leu.2008.310).
Abstract
The FIP1L1-PDGFRA fusion gene is a recurrent molecular abnormality in patients with eosinophilia-associated myeloproliferative neoplasms. We characterized FIP1L1-PDGFRA junction sequences from 113 patients at the mRNA (n=113) and genomic DNA (n=85) levels. Transcript types could be assigned in 109 patients as type A (n=50, 46%) or B (n=47, 43%), which were created by cryptic acceptor splice sites in different introns of FIP1L1 (type A) or within PDGFRA exon 12 (type B). We also characterized a new transcript type C (n=12, 11%) in which both genomic breakpoints fell within coding sequences creating a hybrid exon without use of a cryptic acceptor splice site. The location of genomic breakpoints within PDGFRA and the availability of AG splice sites determine the transcript type and restrict the FIP1L1 exons used for the creation of the fusion. Stretches of overlapping sequences were identified at the genomic junction site, suggesting that the FIP1L1-PDGFRA fusion is created by illegitimate non-homologous end-joining. Statistical analyses provided evidence for clustering of breakpoints within FIP1L1 that may be related to DNA- or chromatin-related structural features. The variability in the anatomy of the FIP1L1-PDGFRA fusion has important implications for strategies to detect the fusion at diagnosis or for monitoring response to treatment
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More information
Published date: February 2009
Keywords:
FIP1L1, PDGFRA, Eos-MPN
Identifiers
Local EPrints ID: 69713
URI: http://eprints.soton.ac.uk/id/eprint/69713
ISSN: 0887-6924
PURE UUID: e9875800-5f09-498d-852c-b00f119ecf10
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Date deposited: 27 Nov 2009
Last modified: 14 Mar 2024 02:46
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Contributors
Author:
C. Walz
Author:
J. Score
Author:
J. Mix
Author:
D. Cilloni
Author:
C. Roche-Lestienne
Author:
R.F. Yeh
Author:
J.L. Wiemels
Author:
E. Ottaviani
Author:
P. Erben
Author:
A. Hochhaus
Author:
M. Baccarani
Author:
D. Grimwade
Author:
C. Preudhomme
Author:
J. Apperley
Author:
G. Martinelli
Author:
G. Saglio
Author:
A. Reiter
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