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Mononuclear cell subpopulations in preterm and full-term neonates: independent effects of gestational age, neonatal infection, maternal pre-eclampsia, maternal betamethason therapy, and mode of delivery

机译:早产儿和足月儿的单核细胞亚群:胎龄,新生儿感染,母体先兆子痫,母体倍他米松治疗和分娩方式的独立影响

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摘要

Blood samples from 29 preterm (24–32 weeks of gestation) and 21 full-term (37–42 weeks of gestation) neonates were analysed for surface markers of lymphocyte subtypes and macrophages, and the effects of gestational age, neonatal infection, maternal pre-eclampsia, maternal betamethason therapy and mode of delivery were assessed with multiple regression analysis. Gestational age alone had few independent effects (increase in CD3+, CD8+CD45RA+, and CD11α+ cells, and decrease in CD14+, HLA-DR− cells) during the third trimester on the proportions of the immune cell subtypes studied. Neonatal infection and mother's pre-eclampsia had the broadest and very opposite kinds of effects on the profile of immune cells in the blood. Infection of the neonate increased the proportions of several ‘immature’ cells (CD11α−CD20+, CD40+CD19−, and CD14+HLA-DR−), whereas mother's pre-eclampsia decreased the proportions of naive cell types (CD4+CD8+, CD5+CD19+). In addition, neonatal infection increased the proportion of T cells (CD3+, CD3+CD25+, and CD4+/CD8+ ratio, and CD45RA+ cells), while maternal pre-eclampsia had a decreasing effect on the proportion of CD4+ cells, CD4+/CD8+ ratio, and proportions of CD11α+, CD14+ and CD14+HLA-DR+ cells. Maternal betamethason therapy increased the proportion of T cells (CD3+) and macrophages (CD14+, CD14+HLA-DR+), but decreased the proportion of natural killer (NK) cells. Caesarean section was associated with a decrease in the proportion of CD14+ cells. We conclude that the ‘normal range’ of proportions of different mononuclear cells is wide during the last trimester; further, the effect of gestational age on these proportions is more limited than the effects of other neonatal and even maternal factors.
机译:分析了29名早产儿(妊娠24–32周)和21名足月儿(妊娠37–42周)的血液样本中淋巴细胞亚型和巨噬细胞的表面标志物,以及胎龄,新生儿感染,孕产妇的影响子痫,孕妇倍他米松治疗和分娩方式通过多元回归分析进行评估。在妊娠晚期,单独的妊娠年龄对免疫细胞亚型的比例几乎没有独立的影响(CD3 +,CD8 + CD45RA +和CD11α+细胞增加,而CD14 +,HLA-DR-细胞减少)。新生儿感染和母亲先兆子痫对血液中免疫细胞谱的影响范围最广,却截然相反。新生儿感染增加了几种“未成熟”细胞(CD11α-CD20+,CD40 + CD19-和CD14 + HLA-DR-)的比例,而母亲的子痫前期则降低了幼稚细胞类型(CD4 + CD8 +,CD5)的比例+ CD19 +)。此外,新生儿感染增加了T细胞的比例(CD3 +,CD3 + CD25 +和CD4 + / CD8 +比率以及CD45RA +细胞),而母亲先兆子痫对CD4 +细胞的比率,CD4 + / CD8 +比率, CD11α+,CD14 +和CD14 + HLA-DR +细胞的比例。母体倍他米松疗法增加了T细胞(CD3 +)和巨噬细胞(CD14 +,CD14 + HLA-DR +)的比例,但降低了自然杀伤(NK)细胞的比例。剖宫产与CD14 +细胞比例的减少有关。我们得出结论,在最后三个月中,不同单核细胞比例的“正常范围”很宽;此外,胎龄对这些比例的影响比其他新生儿甚至母亲因素的影响更为有限。

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