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Dysregulated integrin αVβ3 and CD47 signaling promotes joint inflammation, cartilage breakdown, and progression of osteoarthritis
Qian Wang, Kazuhiro Onuma, Changhao Liu, Heidi Wong, Michelle S. Bloom, Eileen E. Elliott, Richard R.L. Cao, Nick Hu, Nithya Lingampalli, Orr Sharpe, Xiaoyan Zhao, Dong Hyun Sohn, Christin M. Lepus, Jeremy Sokolove, Rong Mao, Cecilia T. Cisar, Harini Raghu, Constance R. Chu, Nicholas J. Giori, Stephen B. Willingham, Susan S. Prohaska, Zhen Cheng, Irving L. Weissman, William H. Robinson
Qian Wang, Kazuhiro Onuma, Changhao Liu, Heidi Wong, Michelle S. Bloom, Eileen E. Elliott, Richard R.L. Cao, Nick Hu, Nithya Lingampalli, Orr Sharpe, Xiaoyan Zhao, Dong Hyun Sohn, Christin M. Lepus, Jeremy Sokolove, Rong Mao, Cecilia T. Cisar, Harini Raghu, Constance R. Chu, Nicholas J. Giori, Stephen B. Willingham, Susan S. Prohaska, Zhen Cheng, Irving L. Weissman, William H. Robinson
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Research Article Immunology Inflammation

Dysregulated integrin αVβ3 and CD47 signaling promotes joint inflammation, cartilage breakdown, and progression of osteoarthritis

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Abstract

Osteoarthritis (OA) is the leading cause of joint failure, yet the underlying mechanisms remain elusive, and no approved therapies that slow progression exist. Dysregulated integrin function was previously implicated in OA pathogenesis. However, the roles of integrin αVβ3 and the integrin-associated receptor CD47 in OA remain largely unknown. Here, transcriptomic and proteomic analyses of human and murine osteoarthritic tissues revealed dysregulated expression of αVβ3, CD47, and their ligands. Using genetically deficient mice and pharmacologic inhibitors, we showed that αVβ3, CD47, and the downstream signaling molecules Fyn and FAK are crucial to OA pathogenesis. MicroPET/CT imaging of a mouse model showed elevated ligand-binding capacities of integrin αVβ3 and CD47 in osteoarthritic joints. Further, our in vitro studies demonstrated that chondrocyte breakdown products, derived from articular cartilage of individuals with OA, induced αVβ3/CD47-dependent expression of inflammatory and degradative mediators, and revealed the downstream signaling network. Our findings identify a central role for dysregulated αVβ3 and CD47 signaling in OA pathogenesis and suggest that activation of αVβ3 and CD47 signaling in many articular cell types contributes to inflammation and joint destruction in OA. Thus, the data presented here provide a rationale for targeting αVβ3, CD47, and their signaling pathways as a disease-modifying therapy.

Authors

Qian Wang, Kazuhiro Onuma, Changhao Liu, Heidi Wong, Michelle S. Bloom, Eileen E. Elliott, Richard R.L. Cao, Nick Hu, Nithya Lingampalli, Orr Sharpe, Xiaoyan Zhao, Dong Hyun Sohn, Christin M. Lepus, Jeremy Sokolove, Rong Mao, Cecilia T. Cisar, Harini Raghu, Constance R. Chu, Nicholas J. Giori, Stephen B. Willingham, Susan S. Prohaska, Zhen Cheng, Irving L. Weissman, William H. Robinson

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Figure 2

Crucial roles of integrin β3, CD47, and Fyn in the development of mouse osteoarthritis.

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Crucial roles of integrin β3, CD47, and Fyn in the development of mouse ...
(A–C) Representative cartilage degeneration scores in safranin O–stained sections of the medial region of stifle joints from Itgb3+/+ (n = 7) and Itgb3–/– (n = 7) (A), Cd47+/+ (n = 7) and Cd47–/– (n = 7) (B), or Fyn+/+ (n = 7) and Fyn–/– (n = 7) (C) mice 20 weeks after destabilization of the medial meniscus (DMM); and quantification of cartilage degeneration and synovitis. Arrowheads indicate areas of cartilage degeneration. Scale bars in the low-magnification (×4; top) images: 500 μm; scale bars in the high-magnification (×10; bottom) images: 200 μm. Mouse DMM data are mean ± SEM of 1 experiment and are representative of ≥2 independent experiments. NS: P > 0.05; *P < 0.05; **P < 0.01 by Mann-Whitney U test. (D–F) qPCR analysis of relative mRNA expression levels of inflammatory mediators and MMPs in bone marrow–derived macrophages from Itgb3+/+ and Itgb3–/– (D), Cd47+/+ and Cd47–/– (E), and Fyn+/+ and Fyn–/– (F) mice stimulated with lysed WT murine chondrocytes. qPCR data are mean ± SEM of triplicates and are representative of 3 independent experiments. NS: P > 0.01; *P < 0.01; **P < 0.001 by Mann-Whitney U test with multiple-comparison corrections.

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