Receptor Protein Tyrosine Phosphatase Alpha Enhances Rheumatoid Synovial Fibroblast Signaling and Promotes Arthritis in Mice

Stephanie M. Stanford¹, Mattias N. D. Svensson¹, Cristiano Sacchetti¹, Caila A. Pilo¹, Dennis J. Wu¹, William B. Kiosses², Annelie Hellvard³, Brith Bergum³, German R. Aleman Muench¹, Christian Elly¹, Yun-Cai Liu¹, Jeroen den Hertog^4,5, Ari Elson⁶, Jan Sap⁷, Piotr Mydel³, David L. Boyle⁸, Maripat Corr⁸, Gary S. Firestein⁸ and Nunzio Bottini¹, ¹Cellular Biology, La Jolla Institute for Allergy and Immunology, La Jolla, CA, ²The Scripps Research Institute, La Jolla, CA, ³Clinical Science, Broegelmann Research Laboratory, Bergen, Norway, ⁴Hubrecht Institute-Koninklijke Nederlands Akademie van Wetenschappen and University Medical Center Utrecht, Utrecht, Netherlands, ⁵Institute of Biology Leiden, Leiden, Netherlands, ⁶Department of Molecular Genetics, Weizmann Institute of Science, Rehovot, Israel, ⁷Epigenetics and Cell Fate, Université Paris Diderot Sorbonne Paris Cité, Paris, France, ⁸Division of Rheumatology, Allergy and Immunology, University of California at San Diego School of Medicine, La Jolla, CA

Meeting: 2015 ACR/ARHP Annual Meeting

Date of first publication: September 29, 2015

Keywords: Fibroblasts, pathogenesis, rheumatoid arthritis (RA) and synovial cells, synovial fluid

Session Information

Date: Monday, November 9, 2015

Title: Rheumatoid Arthritis - Human Etiology and Pathogenesis II

Session Type: ACR Concurrent Abstract Session

Session Time: 4:30PM-6:00PM

Background/Purpose: Rheumatoid arthritis (RA) fibroblast-like synoviocytes (FLS) promote disease pathogenesis by aggressively invading the joint extracellular matrix. The focal adhesion kinase (FAK) signaling pathway is emerging as a contributor to the anomalous behavior of FLS in this disease. Because the receptor protein tyrosine phosphatase α (RPTPα), encoded by the PTPRA gene, is a key promoter of FAK signaling, we investigated whether RPTPα mediates FLS aggressiveness and joint damage.

Methods: Through RPTPα knockdown with cell-permeable morpholino antisense oligonucleotides, we assessed RA FLS gene expression in response to tumor necrosis factor (TNF) and interleukin 1β (IL-1β) by quantitative PCR, invasion in transwell assays in response to platelet-derived growth factor (PDGF), and activation of signaling pathways by Western blotting of FLS lysates. Arthritis development was examined in mice lacking Ptpra using the K/BxN passive serum transfer model. The contribution of radiosensitive and radioresistant cells to disease was evaluated by reciprocal bone-marrow transplantation. Pharmacological inhibition of RPTPα activity was achieved using a novel cell-permeable peptide.

Results: We found that RPTPα was enriched in the RA synovial lining and expressed in RA FLS. Upon RPTPα knockdown, PDGF-induced invasion of RA FLS was decreased by 49±8% (p<0.0001, Mann-Whitney test). RPTPα knockdown in RA FLS also decreased TNF-induced expression of C-X-C motif chemokine 10 (CXCL10) and matrix metalloproteinase 13 (MMP13) by >80% (p<0.001, Mann-Whitney test), and decreased IL-1β-induced production of IL6, MMP3 and MMP13 by ≥50% (p<0.0001, Mann-Whitney test). These phenotypes correlated with >3-fold increase in phosphorylation of SRC on inhibitory Y527 and decreased phosphorylation of FAK on stimulatory Y397. Treatment of RA FLS with inhibitors of SRC and FAK mimicked the effect of RPTPα knockdown. Ptpra-deficient mice were protected from arthritis development (58±3% decrease in area under the curve [AUC] of ankle swelling, p<0.0001, paired t-test), which we confirmed to be due to radioresistant cells. Importantly, pharmacological inhibition of RPTPα activity decreased TNF-induced expression of CXCL10 in RA FLS by 65±16% and reduced arthritis in mice (32±1% decrease in AUC of ankle swelling, p<0.05, paired t-test).

Conclusion: These data suggest that RPTPα mediates pro-inflammatory and pro-invasive signaling in RA FLS by regulating phosphorylation of SRC and FAK. We also find that knockdown or pharmacological inhibition of RPTPα significantly ameliorates arthritis in an FLS-dependent model of RA, suggesting that inhibition of RPTPα could be a novel therapeutic strategy to target the aggressiveness of FLS in RA.

Disclosure: S. M. Stanford, None; M. N. D. Svensson, None; C. Sacchetti, None; C. A. Pilo, None; D. J. Wu, None; W. B. Kiosses, None; A. Hellvard, None; B. Bergum, None; G. R. A. Muench, None; C. Elly, None; Y. C. Liu, None; J. den Hertog, None; A. Elson, None; J. Sap, None; P. Mydel, None; D. L. Boyle, None; M. Corr, None; G. S. Firestein, None; N. Bottini, None.

To cite this abstract in AMA style:

Stanford SM, Svensson MND, Sacchetti C, Pilo CA, Wu DJ, Kiosses WB, Hellvard A, Bergum B, Muench GRA, Elly C, Liu YC, den Hertog J, Elson A, Sap J, Mydel P, Boyle DL, Corr M, Firestein GS, Bottini N. Receptor Protein Tyrosine Phosphatase Alpha Enhances Rheumatoid Synovial Fibroblast Signaling and Promotes Arthritis in Mice [abstract]. Arthritis Rheumatol. 2015; 67 (suppl 10). https://acrabstracts.org/abstract/receptor-protein-tyrosine-phosphatase-alpha-enhances-rheumatoid-synovial-fibroblast-signaling-and-promotes-arthritis-in-mice/. Accessed .

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