Details

Autor(en) / Beteiligte

• Cox, Jennifer H.
• Starr, Amanda E.
• Kappelhoff, Reinhild
• Yan, Rendi
• Roberts, Clive R.
• Overall, Christopher M.

Titel

Matrix metalloproteinase 8 deficiency in mice exacerbates inflammatory arthritis through delayed neutrophil apoptosis and reduced caspase 11 expression

Ist Teil von

• Arthritis & rheumatology (Hoboken, N.J.), 2010-12, Vol.62 (12), p.3645-3655

Ort / Verlag

Hoboken: Wiley Subscription Services, Inc., A Wiley Company

Erscheinungsjahr

2010

Quelle

Wiley-Blackwell Journals

Beschreibungen/Notizen

• Objective Neutrophil accumulation is balanced by both cell infiltration and cell clearance, the controls of which are pivotal in the pathogenesis of rheumatoid arthritis (RA) and other chronic inflammatory diseases. Of the neutrophil‐specific proteases, matrix metalloproteinase 8 (MMP‐8; also known as neutrophil collagenase or collagenase 2) is traditionally viewed as being crucial for collagen degradation and hence cell migration and infiltration. This study was undertaken to examine the role of MMP‐8 in a murine model of spontaneous RA. Methods MMP‐8−/− mice were backcrossed onto the Fas‐defective MRL/lpr background, a mouse strain characterized by systemic autoimmunity including spontaneous autoimmune arthritis. Arthritis was induced with Freund's complete adjuvant and clinical disease and histologic parameters were assessed. Results MMP‐8−/− mice had earlier and more severe joint inflammation than their MMP‐8+/+ counterparts, coupled with a massive accumulation of neutrophils in synovial tissue, an unexpected result considering the commonly held view that MMP‐8 has important extracellular matrix–degradative functions. Protease and protease inhibitor analysis of MMP‐8−/− mouse neutrophils by CLIP‐CHIP microarray revealed very little additional change in protease levels except for low expression of the apoptosis initiator caspase 11. This was confirmed at the protein level in unstimulated, lipopolysaccharide‐treated, and interferon‐γ–treated MMP‐8−/− mouse neutrophils. Downstream of caspase 11, the activity of the apoptosis executioner caspase 3 was consequently reduced in MMP‐8−/− mouse neutrophils, translating to reduced neutrophil apoptosis and cell accumulation compared with wild‐type mouse cells. Conclusion Our findings indicate that MMP‐8 is not essential for neutrophil migration in arthritis and likely other autoimmune diseases. Rather, MMP‐8 is important for normal rates of neutrophil apoptosis and hence regulates cell clearance. Because MMP‐8 deficiency leads to an exaggerated accumulation of neutrophil infiltrates due to delayed apoptosis and concurrent pathologic changes associated with dramatically increased neutrophil infiltration, MMP‐8 is antiinflammatory and therefore a drug antitarget in the treatment of arthritis.