AI Article Synopsis
- Gravid mice infected with Listeria monocytogenes often cannot clear the infection, leading to pregnancy complications or loss of pregnancy.
- In a study, pregnant mice were inoculated with different doses of Listeria, resulting in lower fetal weights and some embryonic deaths compared to control mice.
- Histopathological examinations revealed that significant placental damage occurred when high levels of bacteria were present, suggesting that an acute infection may negatively impact embryonic development and growth.
Article Abstract
Gravid mice and other rodents inoculated with Listeria monocytogenes typically fail to clear an intrauterine infection and either succumb or expel their intrauterine contents. We took advantage of this property to investigate the effects of an extrauterine infection on parameters of pregnancy success. Pregnant mice were selected for our study if they showed no clinical signs of listeriosis following oral inoculation at 7.5 gestational days (gd), and had no detectable intrauterine colony forming units (cfu) at near term (18.5 gd). The range of oral doses employed was 10⁶-10⁸ cfu per mouse for two listerial serotype strains (4nonb and 1/2a). At all doses, inoculation resulted in a decrease in average near-term (18.5 gd) fetal weight per litter compared to sham inoculated controls. Additionally, embryonic death (indicated by intrauterine resorptions) was exhibited by some inoculated mice but was absent in all sham inoculated animals. In parallel experiments designed to detect possible loss of placental function, gravid uteruses were examined histopathologically and microbiologically 96 h after oral inoculation. Placental lesions were associated with high (> 10⁶), but not low (< 10²) or absent intrauterine cfu. In vitro, mouse embryonic trophoblasts were indistinguishable from mouse enterocytes in terms of their sensitivity to listerial exposure. A model consistent with our observations is one in which products (host or bacterial) generated during an acute infection enter embryos transplacentally and influences embryonic survival and slows normal growth in utero.
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Source |
|---|---|
| http://www.ncbi.nlm.nih.gov/pmc/articles/PMC3743821 | PMC |
| http://journals.plos.org/plosone/article?id=10.1371/journal.pone.0072601 | PLOS |
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