Periodontal disease, which affects the gums and tissues around the teeth, is one of the most common dental disorders globally. Periodontal disease, which is most commonly caused by the growth and deposition of bacterial biofilm around the teeth, can eventually lead to tooth loss if not treated properly.
Periodontal disease,
which is most commonly caused by the growth and deposition of bacterial biofilm
around the teeth, can eventually lead to tooth loss if not treated properly.
Interestingly, the inflammatory effects of periodontal bacteria can extend well
beyond the mouth, resulting in systemic consequences. Several decades of
clinical research have proven that the periodontal pathogen Aggregatibacter
actinomycetemcomitans (A. actinomycetemcomitans) is closely related to the
onset and worsening of rheumatoid arthritis (RA), a serious autoimmune disease
that affects joints. However, what goes down at the molecular level remains
largely unexplored and unclear.
In a recent study
published online on 15 August 2024, in the International Journal of Oral
Science, a research team from Tokyo Medical and Dental University (TMDU) in
Japan sought to fill this knowledge gap through detailed mechanistic studies in
an animal model.
First, the researchers
conducted preliminary experiments to confirm whether A. actinomycetemcomitans
infection influenced arthritis in mice. To this end, they used the collagen
antibody-induced arthritis mouse model, which is a well-established
experimental model that mimics several aspects of RA in humans. They found that
infection with this specific bacterium led to increased limb swelling, cellular
infiltration into the lining of the joints, and higher levels of the
inflammatory cytokine interleukin-1b (IL-1b) within the limbs.
Notably, these symptoms
of increasing RA can be alleviated by injecting clodronate, a chemical
substance that depletes macrophages, a type of immune cell. This showed that
macrophages were implicated in exacerbating RA induced by A
actinomycetemcomitans infection.
Further investigation
using macrophages derived from mouse bone marrow revealed that A.
actinomycetemcomitans infection increased the production of IL-1b. In turn,
this triggered the activation of a multiprotein complex known as the
inflammasome, which plays a key role in initiating and modulating the body's
inflammatory response to infections.
The researchers added
yet one more piece to this puzzle using caspase-11-deficient mice. In these
animals, inflammasome activation due to A actinomycetemcomitans was suppressed.
Most importantly, caspase-11-deficient mice exhibited less deterioration of
arthritis symptoms, hinting at the important role that caspase-11 plays in this
context. "Our research findings provide new insights into the link between
periodontal pathogenic bacteria and the exacerbation of arthritis through
inflammasome activation, offering important information on the long-debated
relationship between periodontal disease and systemic diseases,"
highlights Professor Toshihiko Suzuki, one of the lead authors of the study.
With any luck, these
efforts will contribute to the development of novel therapeutic strategies to
manage RA. "The findings of this research may pave the way for advances in
clinical treatments for RA induced by infection with A. actinomycetemcomitans.
Our suggestion to inhibit inflammasome activation could attenuate the expansion
of inflammation to joints, resulting in a recovery from arthritis
symptoms," says lead author Dr Tokuju Okano. "Moreover, the outcome
of our work could contribute to the development of treatment strategies for not
only arthritis but also other systemic diseases, such as Alzheimer's disease,
which is also related to periodontal pathogenic bacteria," he adds with
eyes set on the future.
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