Maternal modulation of neonatal immune system development.

Omar R Fagoaga, Sandra L Nehlsen-Cannarella
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引用次数: 5

Abstract

Changes in programming of neonatal immune development were effected through maternal immune modulation (Leishmania major inoculation). In progeny of these dams, immune profiles in both blood and spleen were changed throughout the neonatal period and were pronounced after weaning. White blood cell (WBC) and lymphocyte counts in blood of 45-day-old progeny were two-fold less than control animals. In blood, proportions of B cells were greater, while T helpers, Tc/s and NK cells were less than in controls. In contrast, proportions of splenic B and NK cells were greater than controls. But, proportions of all T and Tc/s cells on d20 and 45 were lower than controls. In blood, absolute numbers of all T, Th naïve and Th memory cells were lower than in controls. In contrast, in the spleen, numbers of NK, T and Th naive and memory cells were up to 200% greater than in control pups. Cytokine responses of splenic lymphocytes stimulated through CD3 ligation revealed no difference in IL-4 production. In contrast, IL-2 and IFNgamma were lower on d45 and 5, respectively, in the experimental compared to control mice. These data support the hypothesis that maternal immune events during gestation can modulate the pattern of immune development in offspring.

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母亲对新生儿免疫系统发育的调节。
新生儿免疫发育程序的改变是通过母体免疫调节(主要利什曼原虫接种)来实现的。在这些坝的后代中,血液和脾脏的免疫谱在整个新生儿时期都发生了变化,并在断奶后明显。45日龄后代血液中白细胞(WBC)和淋巴细胞计数比对照动物低2倍。在血液中,B细胞的比例高于对照组,而辅助T细胞、Tc/s和NK细胞的比例低于对照组。脾B细胞和NK细胞比例明显高于对照组。但在第20和45天,所有T和Tc/s细胞的比例均低于对照组。在血液中,所有T、Th naïve和Th记忆细胞的绝对数量低于对照组。脾脏NK、T、Th幼稚细胞和记忆细胞的数量比对照组增加了200%。通过CD3结扎刺激脾淋巴细胞的细胞因子反应显示IL-4的产生无差异。相比之下,实验中IL-2和IFNgamma在第45天和第5天分别低于对照小鼠。这些数据支持怀孕期间母体免疫事件可以调节后代免疫发育模式的假设。
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