Carrasco DR, Sukhdeo K, Protopopova M, et al. Targeted overexpression of the transcription factor XBP-1 in B cells promotes plasma cell and lymphoplasmacytic neoplasms in transgenic mice. Cancer Cell, in press.

The majority of studies to date of human multiple myeloma (MM) cells in vivo have utilized xenograft models. Specifically, human MM cells have been injected subcutaneously into SCID mice in order to evaluate the ability of agents to inhibit tumor cell growth and associated angiogenesis, as well as prolong host survival1-3 . A model in which fluorochrome-labeled human MM cells are injected via the tail vein into SCID mice and then migrate and grow primarily in bone has allowed for gene microarray and proteomic studies in MM cells vs. BM as MM cells bind in the BM milieu, both before and after novel drug treatments4 . Direct injection of MM cells into fetal bone chips implanted subcutaneously into SCID mice (SCID hu model) allows for the study of human MM cells in the context of human extracellular matrix proteins and accessory cells in vivo5 . This model has been refined by injecting fluorochrome-labeled cytokine-dependent MM cells directly into human bone grafts within SCID mice, which allows for evaluation of cellular and gene changes triggered in tumor vs. BM by MM cell binding, both before and after treatment with novel agents6,7 . These models have therefore delineated the genetic changes and sequelae induced when MM cells bind to the BM, and conversely validated the ability of novel agents to abrogate these genetic changes and induce tumor cell cytotoxicity even in the BM milieu.

XBP-1 is a transcription factor required for plasma cell differentiation, which is also highly expressed at a gene and protein level in MM cells vs. normal plasma cells8-10 . Interleukin-6 (IL-6) upregulates both transcript and protein levels of XBP-1 in MM cells; conversely, knockdown of XBP-1 decreases viability and sensitizes MM cells to dexamethasone. The novel agent, 2-methoxyestradiol, downregulates XBP-1 transcripts and protein in MM cells9 , whereas the proteasome inhibitor Bortezomib works, at least in part, by targeting XBP-1 and the unfolded protein response8 .

In this paper, Carrasco and colleagues describe a genetically based model of MM, generated by overexpression of XBP-1 spliced isoform (XBP-1s) in the lymphoid system, which faithfully reflects human MM. Specifically, mice transgenic for Eu-directed XBP-1s develop pathognomonic features of monoclonal gammopathy of unclear significance (MGUS), which progress to MM with time, including serum monoclonal protein, bone marrow plasmacytosis, renal disease, and lytic bone disease. In this model, genomic analysis of premalignant B cells and MM cells showed dysregulation of genes with known relevance to human MM, including cyclin D1, MAF, MAFB, and uncovered pathogenetic insights into MCL-1 and FOS/JUN. This model therefore offers a unique opportunity to identify genetic changes mediating the development of MGUS, as well as the progression to MM. Overlay of additional genetic abnormalities (p16, p53) offers the opportunity to shorten the prolonged latency time of this model and define their role in MM pathogenesis. Finally, this model provides a unique system both for identifying novel targets and validating novel targeted therapies.

1.
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Tassone P, Neri P, Burger R, et al. Combination therapy with IL-6 receptor super-antagonist Sant7 and dexamethasone induces antitumor effects in a novel SCID-hu in vivo model of human multiple myeloma. Clin Cancer Res 2005;11:4251-
8.
Lee AH, Iwakoshi NN, Anderson KC, Glimcher LH. Proteasome inhibitors disrupt the unfolded protein response in myeloma cells. Proc Natl Acad Sci USA 2003;100:9946-
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Chauhan D, Li G, Hideshima T, et al. Identification of genes regulated by 2-methoxyestradiol in multiple myeloma cells using oligonucleotide arrays. Blood 2003;101:3606-
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Munshi N, Hideshima T, Carrasco R, et al. Identification of genes modulated in multiple myeloma using genetically identical twin samples. Blood 2004;103:1799-1806.

Competing Interests

Dr. Anderson indicated no relevant conflicts of interest.