Deregulation of MUM1/IRF4 by chromosomal translocation in multiple myeloma

被引：240

作者：

Iida, S

Rao, PH

Butler, M

Corradini, P

Boccadoro, M

Klein, B

Chaganti, RSK

DallaFavera, R

机构：

[1] COLUMBIA UNIV COLL PHYS & SURG, DEPT PATHOL, DIV ONCOL, NEW YORK, NY 10032 USA

[2] COLUMBIA UNIV COLL PHYS & SURG, DEPT GENET & DEV, DIV ONCOL, NEW YORK, NY 10032 USA

[3] MEM SLOAN KETTERING CANC CTR, CELL BIOL PROGRAM, NEW YORK, NY 10021 USA

[4] MEM SLOAN KETTERING CANC CTR, DEPT HUMAN GENET, NEW YORK, NY 10021 USA

[5] UNIV TURIN, DEPT MED & ONCOL, TURIN, ITALY

[6] UNIV MONTPELLIER, INST MOL GENET, F-34059 MONTPELLIER, FRANCE

来源：

NATURE GENETICS | 1997年 / 17卷 / 02期

关键词：

D O I：

10.1038/ng1097-226

中图分类号：

Q3 [遗传学];

学科分类号：

071007 ; 090102 ;

摘要：

The pathogenesis of multiple myeloma (MM), an incurable tumour causing the deregulated proliferation of terminally differentiated B cells, is unknown(1). Chromosomal translocations (14q1) affecting band 14q32 and unidentified partner chromosomes are common in this tumour, suggesting that they may cause the activation of novel oncogenes(2,3). By cloning the chromosomal breakpoints in an MM cell line, we show that the 14q+ translocation represents a t(6;14)(p25;q32) and that this aberration is recurrent in MM, as it was found in two of eleven MM cell lines, The translocation juxtaposes the immunoglobulin heavy-chain (IgH) locus to MUM1 (multiple myeloma oncogene 1)/IRF4 gene, a member of the interferon regulatory factor (IRF) family known to be active in the control of B-cell proliferation and differentiation, As a result, the MUM1/IRF4 gene is overexpressed-an event that may contribute to tumorigenesis, as MUM1/IRF4 has oncogenic activity in vitro. These findings identify a novel genetic alteration associated with MM, with implications for the pathogenesis and diagnostics of this tumour.

引用

页码：226 / 230

页数：5

共 31 条

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