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孕期对大肠杆菌的免疫反应性。

Immunological responsiveness to Escherichia coli during pregnancy.

作者信息

Kenny J F, Diamond M

出版信息

Infect Immun. 1977 Apr;16(1):174-80. doi: 10.1128/iai.16.1.174-180.1977.

Abstract

To determine whether immunological responsiveness to a bacterial antigen is altered during pregnancy and lactation, Swiss mice (gestation, 19 to 21 days) were studied during early, middle, and late pregnancy and in the early postpartum period. Pregnant and nursing mice, each along with a virgin female littermate control, were injected with 2 x 10(6) heat-killed Escherichia coli and sacrificed 4 days later for the enumeration of splenic anti-E. coli plaque-forming cells (PFC). For 72 4- to 10-day pregnant and control mice ranked together, total PFC per spleen ranged from 0 to 312,650, with 61% of the counts from pregnant animals ranking above the median of 12,700. The mean number of PFC for the pregnant animals was greater than for sister controls in 19 of 23 litters studied (P = 0.001). Responsiveness was also increased for 72 mice tested in later pregnancy. Counts of PFC of 72% of mice 11 to 18 days pregnant were above the median when ranked with those of their controls (P < 0.001). In 18 of 21 litters studied, pregnant animals responded better than littermate controls (P = 0.001). Responses of mice at term (19 to 21 days) were depressed when compared with those of controls, but nursing animals 6 to 9 postpartum responded like virgin animals. Previous studies suggested that low concentrations of estradiol stimulate the mitosis of PFC. To determine if progesterone also increases numbers of PFC, concentrations in a range physiological for pregnancy were added to cultures of spleen cells from male mice injected with E. coli 3 days before. After 24 h of incubation, numbers of PFC in these suspensions were compared to those of the same suspensions incubated without hormone. In 19 of 25 and 48 of 68 suspensions tested at concentrations of 500 pg and 50 ng of progesterone per ml, the numbers of PFC were increased over those of the same suspensions without hormone (P < 0.01). Geometric mean number of PFC for progesterone-treated cells was 45% greater than that for the controls. Findings suggest that female sex hormones, important for the normal growth and differentiation of fetal cells, may also enhance division and/or maturation of immunocompetent cells in the mother.

摘要

为了确定孕期和哺乳期对细菌抗原的免疫反应性是否发生改变,对瑞士小鼠(妊娠期为19至21天)在妊娠早期、中期、晚期以及产后早期进行了研究。将怀孕和哺乳的小鼠,每只与同窝未孕的雌性对照小鼠一起,注射2×10⁶个热灭活的大肠杆菌,并在4天后处死以计数脾脏抗大肠杆菌噬斑形成细胞(PFC)。对于72只4至10天龄的怀孕小鼠和对照小鼠一起统计,每只脾脏的总PFC数范围为0至312,650,其中61%的怀孕动物计数高于中位数12,700。在研究的23窝中,有19窝怀孕动物的PFC平均数高于同窝对照小鼠(P = 0.001)。对妊娠后期测试的72只小鼠的反应性也有所增加。当将11至18天龄怀孕小鼠的72%的PFC计数与对照小鼠的计数一起排序时,高于中位数(P < 0.001)。在研究的21窝中有18窝,怀孕动物的反应比同窝对照小鼠更好(P = 0.001)。足月(19至21天)小鼠的反应与对照相比有所降低,但产后6至9天的哺乳小鼠反应与未孕小鼠相似。先前的研究表明低浓度的雌二醇刺激PFC的有丝分裂。为了确定孕酮是否也增加PFC数量,将处于妊娠生理浓度范围内的孕酮添加到3天前注射了大肠杆菌的雄性小鼠的脾细胞培养物中。孵育24小时后,将这些悬浮液中的PFC数量与未添加激素孵育的相同悬浮液中的PFC数量进行比较。在每毫升孕酮浓度为500 pg和50 ng测试的25份悬浮液中的19份以及68份悬浮液中的48份中,添加激素的悬浮液中的PFC数量比未添加激素的相同悬浮液中的PFC数量增加(P < 0.01)。经孕酮处理的细胞的PFC几何平均数比对照细胞高45%。研究结果表明,对胎儿细胞正常生长和分化很重要的雌性性激素,可能也会增强母体中免疫活性细胞的分裂和/或成熟。

相似文献

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Immunological responsiveness to Escherichia coli during pregnancy.孕期对大肠杆菌的免疫反应性。
Infect Immun. 1977 Apr;16(1):174-80. doi: 10.1128/iai.16.1.174-180.1977.

本文引用的文献

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