AI Article Synopsis
- The immune system is modified during pregnancy to allow for fetal tolerance, which may increase susceptibility to infections in pregnant women compared to non-pregnant women.
- Research shows that plasmacytoid dendritic cells (pDCs) in pregnant women have a slightly lower frequency, but produce more interferon (IFN)-α following stimulation.
- The study finds that co-stimulatory receptors CD54 and CD86 on pDCs are less activated in pregnant women, suggesting this could reduce the effectiveness of adaptive antiviral immune responses during pregnancy.
Article Abstract
Physiological modulation of the immune system is required for foetal tolerance during pregnancy. However, this immune regulation might lead to impaired self-defence against pathogens. Indeed, pregnant women are more susceptible to newly encountered viruses comparing to non-pregnant women, as exemplified by the prevalence of severe complications in pregnant women infected with the pandemic influenza virus in 2009. Plasmacytoid dendritic cells (pDCs) are specialized dendritic cells that recognise viral antigens and initiate both innate and adaptive immune responses. We therefore sought to determine whether the number and/or the functions of peripheral blood pDCs are regulated during pregnancy. pDC maturation and interferon (IFN)-α production were analysed in response to Toll-like receptor (TLR) stimulation of peripheral blood mononuclear cells from pregnant and non-pregnant women. Our results reveal that pDC frequency is slightly decreased, while the IFN-α production in response to TLR stimulation increases during pregnancy. Interestingly, the up-regulation of the co-stimulatory receptors CD54 (ICAM1) and CD86 is significantly decreased in pDCs from pregnant women as compared to controls, suggesting a possible impact on T-cell responses. In conclusion, we propose that the modulation of CD54 and CD86 expression on peripheral blood pDCs during pregnancy might decrease the initiation of adaptive antiviral immune responses.
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| http://dx.doi.org/10.3109/08820139.2012.682243 | DOI Listing |
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