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母乳中的白细胞介素 7 可穿过肠道屏障,调节子代 T 细胞的发育。

Interleukin 7 from maternal milk crosses the intestinal barrier and modulates T-cell development in offspring.

机构信息

Department of Immunology, Imperial College London, London, United Kingdom.

出版信息

PLoS One. 2011;6(6):e20812. doi: 10.1371/journal.pone.0020812. Epub 2011 Jun 30.

Abstract

BACKGROUND

Breastfeeding protects against illnesses and death in hazardous environments, an effect partly mediated by improved immune function. One hypothesis suggests that factors within milk supplement the inadequate immune response of the offspring, but this has not been able to account for a series of observations showing that factors within maternally derived milk may supplement the development of the immune system through a direct effect on the primary lymphoid organs. In a previous human study we reported evidence suggesting a link between IL-7 in breast milk and the thymic output of infants. Here we report evidence in mice of direct action of maternally-derived IL-7 on T cell development in the offspring.

METHODS AND FINDINGS

We have used recombinant IL-7 labelled with a fluorescent dye to trace the movement in live mice of IL-7 from the stomach across the gut and into the lymphoid tissues. To validate the functional ability of maternally derived IL-7 we cross fostered IL-7 knock-out mice onto normal wild type mothers. Subsets of thymocytes and populations of peripheral T cells were significantly higher than those found in knock-out mice receiving milk from IL-7 knock-out mothers.

CONCLUSIONS/SIGNIFICANCE: Our study provides direct evidence that interleukin 7, a factor which is critical in the development of T lymphocytes, when maternally derived can transfer across the intestine of the offspring, increase T cell production in the thymus and support the survival of T cells in the peripheral secondary lymphoid tissue.

摘要

背景

母乳喂养在危险环境中可以预防疾病和死亡,这种效果部分是通过改善免疫功能来实现的。有一种假设认为,母乳中的某些因素可以补充后代不完善的免疫反应,但这并不能解释一系列观察结果,这些结果表明,母乳中母体来源的某些因素可能通过对初级淋巴器官的直接作用来补充免疫系统的发育。在之前的一项人类研究中,我们报告了证据表明母乳中的白细胞介素 7(IL-7)与婴儿的胸腺输出之间存在关联。在这里,我们在小鼠中报告了母体来源的 IL-7 对后代 T 细胞发育的直接作用的证据。

方法和发现

我们使用标记有荧光染料的重组 IL-7 来追踪 IL-7 在活小鼠体内从胃部穿过肠道进入淋巴组织的运动。为了验证母体来源的 IL-7 的功能能力,我们将 IL-7 敲除小鼠交叉寄养在正常野生型母亲身上。胸腺细胞亚群和外周 T 细胞群体明显高于从 IL-7 敲除母亲那里获得母乳的敲除小鼠。

结论/意义:我们的研究提供了直接证据,表明白细胞介素 7(IL-7)是 T 淋巴细胞发育的关键因素,当它来自母体时,可以穿过后代的肠道,增加胸腺中的 T 细胞生成,并支持外周次级淋巴组织中 T 细胞的存活。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/d7c5/3127952/9ddaec8080dc/pone.0020812.g001.jpg

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