School of Clinical and Experimental Medicine (Reproduction, Genes & Development), College of Medical and Dental Sciences, University of Birmingham, Birmingham B15 2TT, UK.
Hum Reprod. 2011 Dec;26(12):3355-65. doi: 10.1093/humrep/der327. Epub 2011 Oct 5.
Human pregnancy offers an immunological challenge for the immunocompetent women accommodating an allogenic fetus, while continuing to combat potentially infectious disease. Cytomegalovirus (CMV) infects the majority of the human population and establishes lifelong persistence, which can lead to the oligoclonal expansion of differentiated T cells. Primary CMV infection and, less commonly, secondary infection during pregnancy can cause fetal disease and morbidity. The balance between maternal immune competence and viral pathogenicity is thus delicately poised. Our objective was to investigate the influence of CMV serostatus on maternal CD8+ T-cell phenotype and cytokine profile in an apparently healthy cohort of pregnant women. Furthermore, we assessed if CMV serostatus modulated changes in CD8 T cells during gestation.
CD8+ T-cell phenotype was investigated in 87 pregnant women with samples obtained both during pregnancy [CMV immunoglobulin G (IgG) + n = 39, CMV IgG- n = 21] and in the early post-natal period (IgG+ n = 16, IgG- n = 11). Multiparameter flow cytometry was used to study T-cell phenotype and HLA-peptide tetramers identified CD8 T cells specific for CMV. Levels of 26 plasma cytokines, chemokines and chemokine receptors were assessed in a separate cohort of 20 women (IgG+ n = 10, IgG- n = 10) followed longitudinally during and after pregnancy.
CMV seropositivity profoundly influenced the T cell repertoire and its dynamics during pregnancy. Naïve CD8+ T-cells (CCR7+CD45RA+) were reduced by 50% in CMV-seropositive women. The proportion of CD45RA effector cells was not increased in CMV-seropositive donors, although this population was more highly differentiated with reduced CD27 and CD28. However, there was a doubling in the proportion of CD45RA+ revertant memory cells (CCR7-CD45RA+) in seropositive donors. Moreover, seropositive women during late pregnancy demonstrated an accumulation of highly differentiated CMV-specific T-cells. T-cell activation independent of CMV was also seen in late pregnancy. No CMV-related changes in plasma cytokines, chemokines or their receptors were observed.
Thus, CMV serostatus is a crucial consideration in studies of T cell memory and differentiation during pregnancy. The reduction in maternal naïve T cells in CMV-seropositive donors could have implications for the maternal response to infections during pregnancy. These findings shed light on the delicate balance between host, fetus and chronic infection during healthy pregnancy and will inform studies in relation to the importance of CMV on maternal and fetal health.
人类妊娠为免疫能力正常的女性提供了一个免疫挑战,因为她们需要容纳异体胎儿,同时继续对抗潜在的传染性疾病。巨细胞病毒(CMV)感染了大多数人类,并建立了终身持续性,这可能导致分化 T 细胞的寡克隆扩增。原发性 CMV 感染,以及在妊娠期间较少发生的继发性感染,可导致胎儿疾病和发病率。因此,母体免疫能力和病毒致病性之间的平衡非常微妙。我们的目的是研究 CMV 血清状态对妊娠期间健康孕妇的母体 CD8+T 细胞表型和细胞因子谱的影响。此外,我们评估了 CMV 血清状态是否调节了妊娠期间 CD8 T 细胞的变化。
我们在 87 名孕妇中研究了 CD8+T 细胞表型,这些孕妇在妊娠期间(CMV 免疫球蛋白 G [IgG]+n=39,CMV IgG-n=21)和产后早期(IgG+n=16,IgG-n=11)均获得了样本。使用多参数流式细胞术研究 T 细胞表型,并使用 HLA 肽四聚体鉴定 CMV 特异性 CD8 T 细胞。在另一项包括 20 名女性(IgG+n=10,IgG-n=10)的队列中,我们在妊娠期间和之后进行了纵向评估,以评估 26 种血浆细胞因子、趋化因子和趋化因子受体的水平。
CMV 血清阳性显著影响了 T 细胞库及其在妊娠期间的动态变化。CMV 血清阳性的女性中,幼稚 CD8+T 细胞(CCR7+CD45RA+)减少了 50%。在 CMV 血清阳性供体中,CD45RA 效应细胞的比例没有增加,尽管这些细胞群的分化程度更高,CD27 和 CD28 减少。然而,在血清阳性供体中,CD45RA+恢复记忆细胞(CCR7-CD45RA+)的比例增加了一倍。此外,在妊娠晚期,血清阳性的女性表现出高度分化的 CMV 特异性 T 细胞的积累。在妊娠晚期也观察到与 CMV 无关的 T 细胞激活。未观察到与 CMV 相关的血浆细胞因子、趋化因子或其受体的变化。
因此,CMV 血清状态是研究妊娠期间 T 细胞记忆和分化的一个重要考虑因素。CMV 血清阳性供体中母源幼稚 T 细胞的减少可能对孕妇在妊娠期间对感染的母体反应产生影响。这些发现揭示了健康妊娠期间宿主、胎儿和慢性感染之间微妙平衡,将为与 CMV 对母婴健康重要性相关的研究提供信息。
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