AI Article Synopsis
- IL-17A plays a role in forming lung granulomas during TB infections by attracting neutrophils, but its protective effects vary based on the infection's severity.
- In experiments with high doses of the less virulent Mtb strain H37rv, mice lacking IL-17A showed increased vulnerability due to unchecked bacterial growth within neutrophils.
- The observed susceptibility in IL-17A-deficient mice was linked to IL-17F compensating for IL-17A absence, highlighting the complex role of Th17 cytokines in TB and the negative impact of too many neutrophils in response to the bacteria.
Article Abstract
During experimental tuberculosis (TB), interleukin (IL)-17A appears to be involved in the formation of lung granulomas, possibly through the attraction of neutrophils to the sites of infection. However, the protective impact of cytokine appears to depend on the degree of its induction. Hence, robust production of IL-17A in mice infected with the hypervirulent isolate (Mtb) HN878 mediates protection, while the cytokine is dispensable for protective immune responses against low-dose infection with the less virulent strain H37rv. Here, we show that after experimental infection with high doses of Mtb H37rv, IL-17A-deficient () mice exhibited high susceptibility to the infection, which was mediated by the strong accumulation of neutrophils in the infected lung tissue. Accordingly, we observed nearly unrestricted bacterial replication within the neutrophils, indicating that they may serve as a survival niche for Mtb. By use of IL-17A/IL-17F-double-deficient mice, we demonstrated that the susceptibility in the absence of IL-17A is mediated by a compensatory expression of IL-17F, which, however, appeared not to be dependent on neutrophils. Together, our results illustrate the compensatory potential of the Th17-secreted cytokines IL-17A and IL-17F in the context of experimental TB and once again emphasize the detrimental effect of excessive neutrophil infiltration in response to Mtb.
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| http://www.ncbi.nlm.nih.gov/pmc/articles/PMC9496946 | PMC |
| http://dx.doi.org/10.3390/cells11182875 | DOI Listing |
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