Gallinarum only infects avian species, where it causes a severe systemic infection in birds of all ages. It is generally accepted that interaction with phagocytic cells plays an important role in the development of systemic, host-specific infections. The current study detailed the interaction of . Gallinarum with macrophages derived from chicken (HD11) and cattle (Bomac) compared to interaction of the broad host range serovar, Typhimurium and the cattle adapted serovar Dublin. Results showed a weaker invading ability of . Gallinarum in both kinds of macrophages, regardless whether the bacteria were opsonized or not before infections. However, opsonization of . Gallinarum by chicken serum increased its intracellular survival rate in chicken macrophages. No significant induction of nitrogen oxide was observed in the infected HD11 cells within the first 6 h, and levels of reactive oxygen species (ROS) were similar among the three serovars. . Gallinarum infection was associated with low cell deaths in both chicken and cattle macrophages, whereas . Dublin only induced a comparable high level of cell death in chicken macrophages, but not in macrophages of its preferred host species (Bomac) compared to host generalist . Typhimurium. . Gallinarum-infected HD11 macrophages exhibited low induction of pro-inflammation genes [interleukin (IL)1β, CXCLi1, and CXCLi2] compared to the two other serovars, and contrary to the other serovars, it did not induce significant downregulation of Toll-like receptor (TLR)2, TLR4, and TLR5. In infection of 1-week-old chicken, a significant upregulation of the TLR4 and TLR5 genes in the spleen was observed in . Gallinarum-infected chickens, but not in . Typhimurium-infected chicken at 5 days post-infections. Taken together, results show that . Gallinarum infection of macrophages was characterized by low uptake and low cytotoxicity, possibly allowing long-term persistence in the intracellular environment, and it caused a low induction of pro-inflammatory responses.
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| http://dx.doi.org/10.3389/fcimb.2019.00420 | DOI Listing |
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