To better define the molecular basis of multiple myeloma (MM), we performed unsupervised hierarchic clustering of mRNA expression profiles in CD138-enriched plasma cells from 414 newly diagnosed patients who went on to receive high-dose therapy and tandem stem cell transplants. Seven disease subtypes were validated that were strongly influenced by known genetic lesions, such as c-MAF-and MAFB-, CCND1-and CCND3-, and MMSET-activating translocations and hyperdiploidy. Indicative of the deregulation of common pathways by gene orthologs, common gene signatures were observed in cases with c-MAF and MAFB activation and CCND1 and CCND3 activation, the latter consisting of 2 subgroups, one characterized by expression of the early B-cell markers CD20 and PAX5. A low incidence of focal bone disease distinguished one and increased expression of proliferation-associated genes of another novel subgroup. Comprising varying fractions of each of the other 6 subgroups, the proliferation subgroup dominated at relapse, suggesting that this signature is linked to disease progression. Proliferation and MMSET-spike groups were characterized by significant overexpression of genes mapping to chromosome 1q, and both exhibited a poor prognosis relative to the other groups. A subset of cases with a predominating myeloid gene expression signature, excluded from the profiling analyses, had more favorable baseline characteristics and superior prognosis to those lacking this signature.
IntroductionMultiple myeloma (MM) is a malignancy of antibody-secreting, terminally differentiated B cells that home to and expand in the bone marrow, with symptoms related to anemia, immunosuppression, bone destruction, and renal failure. 1,2 Bone lesions developing adjacent to plasma cell foci result from the activation of osteoclasts and inactivation of osteoblasts. [3][4][5] Many of the pathogenetic mechanisms of this clinically heterogeneous malignancy have been unraveled by application of molecular genetics. [6][7][8] While sharing most of the genetic lesions seen in MM, 9-11 monoclonal gammopathy of undetermined significance (MGUS) rarely progresses to overt MM. 12 The universal activation of 1 of the 3 cyclin D genes is consistent with this being an initiating event in MM. 13 Nonhyperdiploid MM, present in 40%, is characterized by transcriptional activation of CCND1, CCND3, MAF, MAFB, or FGFR3/MMSET genes (resulting from translocations involving the immunoglobulin heavy chain locus). 8 While hyperdiploidy and CCND1 activation confer a favorable prognosis, MAF, MAFB, or FGFR3/MMSET activation and deletion of chromosomes 13 and 17 are associated with poor prognosis. [14][15][16][17][18][19][20][21][22][23][24][25] Although high-dose therapy has markedly improved MM prognosis, 26-28 individual patients' survival remains variable 29,30 and cannot be accurately predicted with current prognostic models. 31,32 In lymphoma and leukemia, microarray profiling has helped establish clinically relevant disease subclassifications. [33][34][35][36][37][38][39][40][41...
