Translocations at 8q24 juxtapose MYC with genes that harbor superenhancers resulting in overexpression and poor prognosis in myeloma patients
Translocations at 8q24 juxtapose MYC with genes that harbor superenhancers resulting in overexpression and poor prognosis in myeloma patients
Secondary MYC translocations in myeloma have been shown to be important in the pathogenesis and progression of disease. Here, we have used a DNA capture and massively parallel sequencing approach to identify the partner chromosomes in 104 presentation myeloma samples. 8q24 breakpoints were identified in 21 (20%) samples with partner loci including IGH, IGK and IGL, which juxtapose the immunoglobulin (Ig) enhancers next to MYC in 8/23 samples. The remaining samples had partner loci including XBP1, FAM46C, CCND1 and KRAS, which are important in B-cell maturation or myeloma pathogenesis. Analysis of the region surrounding the breakpoints indicated the presence of superenhancers on the partner chromosomes and gene expression analysis showed increased expression of MYC in these samples. Patients with MYC translocations had a decreased progression-free and overall survival. We postulate that translocation breakpoints near MYC result in colocalization of the gene with superenhancers from loci, which are important in the development of the cell type in which they occur. In the case of myeloma these are the Ig loci and those important for plasma cell development and myeloma pathogenesis, resulting in increased expression of MYC and an aggressive disease phenotype
e191
Walker, B.A.
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Wardell, C.P.
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Brioli, A.
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Boyle, E.
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Kaiser, M.F.
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Begum, D.B.
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Dahir, N.B.
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Johnson, D.C.
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Ross, F.M.
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Davies, F.E.
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Morgan, G.J.
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Walker, B.A.
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Wardell, C.P.
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Brioli, A.
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Boyle, E.
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Kaiser, M.F.
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Begum, D.B.
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Dahir, N.B.
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Johnson, D.C.
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Ross, F.M.
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Davies, F.E.
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Morgan, G.J.
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Walker, B.A., Wardell, C.P., Brioli, A., Boyle, E., Kaiser, M.F., Begum, D.B., Dahir, N.B., Johnson, D.C., Ross, F.M., Davies, F.E. and Morgan, G.J.
(2014)
Translocations at 8q24 juxtapose MYC with genes that harbor superenhancers resulting in overexpression and poor prognosis in myeloma patients.
Blood Cancer Journal, 4 (3), .
(doi:10.1038/bcj.2014.13).
(In Press)
Abstract
Secondary MYC translocations in myeloma have been shown to be important in the pathogenesis and progression of disease. Here, we have used a DNA capture and massively parallel sequencing approach to identify the partner chromosomes in 104 presentation myeloma samples. 8q24 breakpoints were identified in 21 (20%) samples with partner loci including IGH, IGK and IGL, which juxtapose the immunoglobulin (Ig) enhancers next to MYC in 8/23 samples. The remaining samples had partner loci including XBP1, FAM46C, CCND1 and KRAS, which are important in B-cell maturation or myeloma pathogenesis. Analysis of the region surrounding the breakpoints indicated the presence of superenhancers on the partner chromosomes and gene expression analysis showed increased expression of MYC in these samples. Patients with MYC translocations had a decreased progression-free and overall survival. We postulate that translocation breakpoints near MYC result in colocalization of the gene with superenhancers from loci, which are important in the development of the cell type in which they occur. In the case of myeloma these are the Ig loci and those important for plasma cell development and myeloma pathogenesis, resulting in increased expression of MYC and an aggressive disease phenotype
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Accepted/In Press date: March 2014
Organisations:
Human Development & Health
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Local EPrints ID: 363259
URI: http://eprints.soton.ac.uk/id/eprint/363259
ISSN: 2044-5385
PURE UUID: d183211a-7e0b-4681-8481-73885f311062
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Date deposited: 24 Mar 2014 11:01
Last modified: 14 Mar 2024 16:21
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Author:
B.A. Walker
Author:
C.P. Wardell
Author:
A. Brioli
Author:
E. Boyle
Author:
M.F. Kaiser
Author:
D.B. Begum
Author:
N.B. Dahir
Author:
D.C. Johnson
Author:
F.M. Ross
Author:
F.E. Davies
Author:
G.J. Morgan
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