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IFN‐alpha receptor deficiency enhances host resistance to oral Salmonella enterica serovar Typhimurium infection during murine pregnancy
Author(s) -
Agbayani Gerard,
Clark Kristina,
Sandhu Jagdeep K.,
Hewitt Melissa,
Sad Subash,
Murphy Shawn P.,
Krishnan Lakshmi
Publication year - 2021
Publication title -
american journal of reproductive immunology
Language(s) - English
Resource type - Journals
SCImago Journal Rank - 1.071
H-Index - 97
eISSN - 1600-0897
pISSN - 1046-7408
DOI - 10.1111/aji.13454
Subject(s) - biology , salmonella enterica , placenta , pregnancy , spleen , inflammation , salmonella infection , immunology , tumor necrosis factor alpha , fetus , gestation , salmonella , bacteria , genetics
Problem Maternal tolerance during pregnancy increases the risk of infection with certain intracellular pathogens. Systemic Salmonella enterica serovar Typhimurium ( S .Tm) infection during pregnancy in normally resistant 129X1/SvJ mice leads to severe placental infection, as well as fetal and maternal deaths. However, the effect of oral infection with S .Tm in pregnant mice and the roles of infection‐induced inflammation and cell death pathways in contributing to susceptibility to infection are unclear. Method of Study Non‐pregnant and pregnant C57BL/6J wild‐type (WT) and cell death pathway‐altered mice (IFNAR1 −/− , Caspase‐1, 11 −/− , RIP3 −/− ) were infected orally with S .Tm. Host survival and fetal resorption were determined. Bacterial burden in mesenteric lymph nodes (MLNs), spleen, liver, and placentas was enumerated at various time points post‐infection. Serum cytokine expression was measured through cytometric bead array. Results Oral infection of WT mice with S .Tm on days 9–10 of gestation resulted in systemic dissemination of the bacteria, substantial placental colonization, and fetal loss 5 days post‐infection. Histopathological examination of the placentas indicated that infection‐induced widespread focal necrosis and neutrophil infiltration throughout the spongiotrophoblast (SpT) layer. In the non‐pregnant state, IFNAR1 −/− mice exhibited increased survival following oral S .Tm infection relative to Caspase‐1, 11 −/− , RIP3 −/− , and WT mice. The increased resistance to S .Tm infection in IFNAR1 −/− mice was seen during pregnancy as well, with decreased bacterial burden within MLNs, spleen, and placenta, which correlated with the decreased resorptions relative to WT and Caspase‐1, 11 −/− mice. Conclusion Oral S .Tm exposure leads to placental infection, inflammation, and resorption, whereas IFNAR1 deficiency enhances host resistance both in the non‐pregnant and pregnant states.