Multiple myeloma–derived MMP-13 mediates osteoclast fusogenesis and osteolytic disease
Jing Fu, … , Stephen J. Weiss, Suzanne Lentzsch
Jing Fu, … , Stephen J. Weiss, Suzanne Lentzsch
Published April 4, 2016
Citation Information: J Clin Invest. 2016;126(5):1759-1772. https://doi.org/10.1172/JCI80276.
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Research Article Oncology

Multiple myeloma–derived MMP-13 mediates osteoclast fusogenesis and osteolytic disease

Abstract

Multiple myeloma (MM) cells secrete osteoclastogenic factors that promote osteolytic lesions; however, the identity of these factors is largely unknown. Here, we performed a screen of human myeloma cells to identify pro-osteoclastogenic agents that could potentially serve as therapeutic targets for ameliorating MM-associated bone disease. We found that myeloma cells express high levels of the matrix metalloproteinase MMP-13 and determined that MMP-13 directly enhances osteoclast multinucleation and bone-resorptive activity by triggering upregulation of the cell fusogen DC-STAMP. Moreover, this effect was independent of the proteolytic activity of the enzyme. Further, in mouse xenograft models, silencing MMP-13 expression in myeloma cells inhibited the development of osteolytic lesions. In patient cohorts, MMP-13 expression was localized to BM-associated myeloma cells, while elevated MMP-13 serum levels were able to correctly predict the presence of active bone disease. Together, these data demonstrate that MMP-13 is critical for the development of osteolytic lesions in MM and that targeting the MMP-13 protein — rather than its catalytic activity — constitutes a potential approach to mitigating bone disease in affected patients.

Authors

Jing Fu, Shirong Li, Rentian Feng, Huihui Ma, Farideh Sabeh, G. David Roodman, Ji Wang, Samuel Robinson, X. Edward Guo, Thomas Lund, Daniel Normolle, Markus Y. Mapara, Stephen J. Weiss, Suzanne Lentzsch

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Figure 7

BM and serum MMP-13 levels in MM patients.

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BM and serum MMP-13 levels in MM patients. (A) Tissue arrays of normal c...
(A) Tissue arrays of normal costal tissue (top panel, n = 10) and of tissue from MM patients (bottom panel, n = 11) were subjected to immunohistochemical staining using an hMMP-13 Ab. Scale bars: 20 μm. (B) MMP-13 levels in sera from healthy donors (n = 6) and from MM patients with bone disease (MMBD) (n = 18) and without MMBD (n = 14) were determined by ELISA. *P ≤ 0.05 and **P ≤ 0.01, by 2 Wilcoxon rank-sum tests with Bonferroni’s correction. (C) Role of MMP-13 in MM: IL-6 expressed in the BM microenvironment induces MMP-13 secretion from MM cells. MMP-13 subsequently activates ERK1/2 signaling in OCL precursors and mediates the subsequent induction of NFATc1 and DC-STAMP expression, resulting in enhanced OCL fusion, activity, and osteolysis.