Tumor necrosis factor-interleukin-17 interplay induces S100A8, interleukin-1β, and matrix metalloproteinases, and drives irreversible cartilage destruction in murine arthritis: rationale for combination treatment during arthritis

Marije I Koenders; Renoud J Marijnissen; Isabel Devesa; Erik Lubberts; Leo A B Joosten; Johannes Roth; Peter L E M van Lent; Fons A van de Loo; Wim B van den Berg

doi:10.1002/art.30418

Tumor necrosis factor-interleukin-17 interplay induces S100A8, interleukin-1β, and matrix metalloproteinases, and drives irreversible cartilage destruction in murine arthritis: rationale for combination treatment during arthritis

Arthritis Rheum. 2011 Aug;63(8):2329-39. doi: 10.1002/art.30418.

Authors

Marije I Koenders¹, Renoud J Marijnissen, Isabel Devesa, Erik Lubberts, Leo A B Joosten, Johannes Roth, Peter L E M van Lent, Fons A van de Loo, Wim B van den Berg

Affiliation

¹ Radboud University Nijmegen Medical Centre, Department of Rheumatology, Nijmegen, The Netherlands. m.koenders@reuma.umcn.nl

PMID: 21520013
DOI: 10.1002/art.30418

Abstract

Objective: To examine whether synovial interleukin-17 (IL-17) expression promotes tumor necrosis factor (TNF)-induced joint pathologic processes in vivo, and to analyze the surplus ameliorative value of neutralizing IL-17 in addition to TNF during collagen-induced arthritis (CIA).

Methods: Adenoviral vectors were used to induce overexpression of IL-17 and/or TNF in murine knee joints. In addition, mice with CIA were treated, at different stages of arthritis, with soluble IL-17 receptor (sIL-17R), TNF binding protein (TNFBP), or the combination.

Results: Overexpression of IL-17 and TNF resulted in joint inflammation and bone erosion in murine knees. Interestingly, IL-17 strikingly enhanced both the joint-inflammatory and joint-destructive capacity of TNF. Further analysis revealed a strongly enhanced up-regulation of S100A8, IL-1β, and matrix metalloproteinase (MMP) messenger RNA, only when both TNF and IL-17 were present. Moreover, the increase in irreversible cartilage destruction was not merely the result of enhanced inflammation, but also was associated with a direct synergistic effect of these cytokines in the joint. S100A9 deficiency in mice protected against IL-17/TNF-induced expression of cartilage NITEGE neoepitopes. During established arthritis, the combination of sIL-17R and TNFBP was more effective than the anticytokine treatments alone, and significantly inhibited further joint inflammation and cartilage destruction.

Conclusion: Local synovial IL-17 expression enhances the role of TNF in joint destruction. Synergy between TNF and IL-17 in vivo results in striking exaggeration of cartilage erosion, in parallel with a synergistic up-regulation of S100A8, IL-1β, and erosive MMPs. Moreover, neutralizing IL-17 in addition to TNF further improves protection against joint damage and is still effective during late-stage CIA. Therefore, compared with anti-TNF alone, combination blocking of TNF and IL-17 may have additional therapeutic value for the treatment of destructive arthritis.

Publication types

Research Support, Non-U.S. Gov't

MeSH terms

Animals
Arthritis, Experimental / metabolism*
Arthritis, Experimental / pathology
Calgranulin A / metabolism*
Cartilage, Articular / metabolism*
Cartilage, Articular / pathology
Interleukin-17 / metabolism*
Interleukin-1beta / metabolism*
Knee Joint / metabolism
Knee Joint / pathology
Male
Matrix Metalloproteinases / metabolism*
Mice
Mice, Transgenic
Tumor Necrosis Factor-alpha / metabolism*

Substances

Calgranulin A
Interleukin-17
Interleukin-1beta
Tumor Necrosis Factor-alpha
Matrix Metalloproteinases