Abstract:
Introduction. Reactive Arthritis(ReA) is an immune-mediated synovitis resulting from slow
bacterial infections and showing intra-articular persistence of viable nonculturable bacteria
and/or immunogenetic bacterial antigens synthesized by metabolically active bacteria residing
in the joint and/or elsewhere in the body.Reactive arthritis is known to be triggered by a
bacterial infection, particularly of the genitourinary (Chl. trachomatis, Neisseria gonorrhea,
Mycoplasma hominis, and Ureaplasma urealyticum) or GI tract (Salmonella enteritidis,
Shigella flexneri, and disenteriae, Yersinia enterocolitica, Campylobacter jejuni, Cl.difficile).
The incidence is about 2% to 4% after a urogenital infection mainly with chlamydia
trachomatis and varies from 0% to 15% after gastrointestinal infections with Salmonella,
Shigella, Campylobacter, or Yersinia.
Aim of the study. To identify the most common infections that lead to the reactive arthritis
and to highlight the pathogenetic mechanisms of action, which would help to improve the
treatment tactic.
Materials and methods. The relevant articles on the topic were taken from the databases
NCBI, PubMed, Medline,and ScienceDirect .
Results. Reactive arthritis is an immune-mediated syndrome triggered by a recent infection. It
is hypothesized that when the invasive bacteria reach the systemic circulation, T lymphocytes
are induced by bacterial fragments such as lipopolysaccharide and nucleic acids. These
activated cytotoxic-T cells then attack the synovium and other self-antigens through molecular
mimicry. This is supported by the evidence of Chlamydia trachomatis and C pneumoniae
ribosomal RNA transcripts, enteric bacterial DNA and bacterial degradation products in the
synovial tissue and fluid. It is believed that anti-bacterial cytokine response is also impaired in
reactive arthritis, resulting in the decreased elimination of the bacteria.
Conclusions. Current evidence supports the concept that reactive arthritis (ReA) is an
immune-mediated synovitis resulting from slow bacterial infections and showing intraarticular
persistence of viable, nonculturable bacteria and/or immunogenetic bacterial antigens
synthesized by metabolically active bacteria residing in the joint and/or elsewhere in the body.
The mechanisms that lead to the development of ReA are complex and basically involve an
interaction between an arthritogenic agent and a predisposed host. The way in which a host
accommodates to invasive facultative intracellular bacteria is the key to the development of
ReA. The details of the molecular pathways that explain the articular and extra-articular
manifestations of the disease are still under investigation.
Description:
Department of Internal
Medicine: Rheumatology and Nephrology, Nicolae Testemitanu State University of Medicine
and Pharmacy, Chisinau, Republic of Moldova, The 8th International Medical Congress for Students and Young Doctors, September 24-26, 2020