Rheumatoid arthritis is an autoimmune disease that causes pain, swelling and damage of the joints. It is the second most common form of arthritis in the UK, more frequently affecting women than men, at a ratio of 3:1. The disease is characterised by persistent high levels of inflammation generated by activated immune cells that infiltrate the joints and release cytokines. This causes damage to the soft tissue, cartilage and bone causing deformity and loss of function. In addition, more widespread inflammation can occur which affects other parts of the body leading to complications of cardiovascular disease, fatigue and depression.
Research into rheumatoid arthritis seeks to improve our understanding of the disease mechanisms and treatment strategies with the ultimate aim of translating cutting-edge research into clinical practice.
The mechanisms that drive the persistent inflammation in rheumatoid arthritis are not fully understood. The inflammatory cytokines TNF and IL-6 are known to be important in maintaining the inflammation and joint damage. However, the pathways driving the production of these cytokines are still under investigation.
Potential candidates that may activate these pathways in rheumatoid arthritis are the toll-like receptors, a family of innate immune receptors and researchers at the University of Â鶹¹û¶³´«Ã½ demonstrated a potential role for these receptors in experimental arthritis models of arthritis and in cultures of human rheumatoid arthritis joint tissue. The studies aimed at investigating the expression, function and regulation of these receptors in immune cells from rheumatoid arthritis patients compared to healthy volunteers.
Novel targets for the treatment of rheumatoid arthritis
Traditionally, rheumatoid arthritis is treated clinically with anti-inflammatory drugs. In the twenty-first century, the clinical management of the disease has been improved substantially by the introduction of antibodies that target inflammatory cytokines or their receptors.However, the use of these therapies is limited because they are expensive. Also, the global suppression of cytokine function increases the potential for bacterial and fungal infections. In addition, not all patients respond to these therapies and some patients become unresponsive to treatment over time.
Reseaerchers have discovered an off-target anti-inflammatory effect of anti-depressant drugs. In experimental arthritis models these drugs can inhibit the progress of the disease and can reduce inflammatory cytokine production from human rheumatoid arthritis joint tissue. These drugs indicated the potential to produce new therapies for rheumatoid arthritis in the future.
To achieve this goal, the mechanism by which these drugs are anti-inflammatory will need to be identified. Work is currently ongoing to uncover the exact target that the drugs interact with to generate the anti-inflammatory effect. Identification of the target will facilitate the design of potential new therapies for rheumatoid arthritis.
Non-joint symptoms of rheumatoid arthritis
Fatigue is one of the most common and debilitating symptoms experienced by patients with rheumatoid arthritis. However, little is known about how it is caused or how best to treat it. Interestingly, some treatments designed to reduce rheumatoid arthritis joint inflammation also dramatically reduce fatigue. How these medications reduce fatigue or why they work in only a fraction of the patients however is poorly understood.
Researchers have been investigating how these anti-inflammatory medications reduce fatigue using a combination of brain imaging, sleep recordings, questionnaires and measures of peripheral inflammation, for example using functional magnetic resonance imaging (fMRI) to show that feelings of fatigue appear to be due to activation of a specific immune brain communication pathway. Among the research hypotheses tested have been tests as to whether anti-inflammatory medications improved fatigue in rheumatoid arthritis by deactivating this pathway.
Understanding the mechanisms of rheumatoid arthritis fatigue offers the potential to develop targeted therapies for this common, highly disabling and presently neglected symptom. It may also help determine why these therapies are more helpful for treating fatigue in some patients than others.