Abstract
Objective
The role of innate immunity in Chlamydia‐induced arthritis has not been defined. The purpose of this study was to examine the role of neutrophils in experimental arthritis in mice with targeted elimination of the small GTPases Rac1 and Rac2, as well as the role of Toll‐like receptors (TLRs) in this model.
Methods
Arthritis was induced by intraarticular inoculation of synoviocyte‐packaged Chlamydia trachomatis. The degree of arthritis was assessed according to joint swelling and pathology scores. The persistence of Chlamydia in joints was assessed by immunoassay. The expression of TLR‐2 and TLR‐4 in neutrophils was detected by semiquantitative reverse transcription–polymerase chain reaction.
Results
In the acute phase, wild‐type mice developed more severe arthritis than did Rac‐deficient mice, with abundant infiltration of neutrophils into the joint. In the chronic phase, the Rac‐deficient mice developed more severe arthritis and demonstrated defective clearance of the pathogen from the joint. In vitro stimulation of neutrophils with Chlamydia up‐regulated the expression of TLR‐4, but not TLR‐2, in wild‐type mice. However, neutrophils from Rac‐deficient mice did not show this up‐regulation of TLR‐4. Sustained TLR‐4 expression in neutrophils was found to be dependent on the expression of Rac. Mice genetically deficient in TLR‐4 demonstrated more severe arthritis than did the controls. Thus, Rac expression plays a profound role in infection‐triggered arthritis and demonstrates a bimodal influence on the disease process, exacerbating acute joint inflammation but controlling chronic arthritis. Rac deficiency was associated with diminished TLR‐4 expression, impaired host clearance of the pathogen, and more severe chronic arthritis.
Conclusion
In infection‐triggered arthritis, innate immunity plays a critical role. Effective host clearance of an arthritogenic pathogen depends on intact expression of Rac and appropriate expression of TLR‐4 by neutrophils.