AI Article Synopsis

  • This study focuses on the role of neutrophils in the innate immune response to tuberculosis, specifically how they respond during treatment of the disease.
  • Researchers isolated neutrophils from both healthy individuals and pulmonary tuberculosis patients and evaluated changes in specific receptors (TLR2 and TLR4) and cytokine production over the course of treatment.
  • The findings revealed an increase in TLR2 expression in tuberculosis patients throughout therapy and a fluctuating pattern of certain chemokines, suggesting that neutrophils play a complex role in combating tuberculosis and warrant further investigation.

Article Abstract

Host innate immune responses to tuberculosis are poorly explored. Recent findings emphasize the importance of innate cells in working against Mycobacterium tuberculosis, the etiologic agent of this deadly disease. In this study we have tried to learn the role of neutrophils in building up immunity against this pathogen during therapy. We isolated neutrophils from peripheral blood of healthy volunteers and pulmonary tuberculosis patients at different phases of their treatment and cultured them withtoll like receptor ligands overnight. Toll like receptor 2 and 4 expression on neutrophils was analyzed using flow cytometry. The supernatants were used to measure cytokines. We found that in tuberculosis patients, expression of TLR2, a proven receptor of Mycobacterium tuberculosis on neutrophils, was increased throughout the duration of therapy (measured at diagnosis, second month and sixth month of therapy). This demonstrates that TLR2 expression is altered as a result of treatment, but not TLR4. Also, the chemokines IL-8 and MIP1α showed a 'dip and raise' fashion as the therapy proceeded. Even though the increase in the pro-inflammatory cytokine secretion by neutrophils seen at the end of therapy is not as expected, it definitely increases our understanding on the function of these cells during TB disease and its resolution and opens new direction in neutrophil research.

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http://dx.doi.org/10.1016/j.molimm.2021.10.009DOI Listing

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