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从鼠 T 细胞库中洞察免疫系统的发育和功能。

Insights into immune system development and function from mouse T-cell repertoires.

机构信息

Joseph Henry Laboratories, Princeton University, Princeton, NJ 08544.

Laboratoire de Physique Théorique, UMR8549, CNRS, École Normale Supérieure, 75005 Paris, France.

出版信息

Proc Natl Acad Sci U S A. 2017 Feb 28;114(9):2253-2258. doi: 10.1073/pnas.1700241114. Epub 2017 Feb 14.

Abstract

The ability of the adaptive immune system to respond to arbitrary pathogens stems from the broad diversity of immune cell surface receptors. This diversity originates in a stochastic DNA editing process (VDJ recombination) that acts on the surface receptor gene each time a new immune cell is created from a stem cell. By analyzing T-cell receptor (TCR) sequence repertoires taken from the blood and thymus of mice of different ages, we quantify the changes in the VDJ recombination process that occur from embryo to young adult. We find a rapid increase with age in the number of random insertions and a dramatic increase in diversity. Because the blood accumulates thymic output over time, blood repertoires are mixtures of different statistical recombination processes, and we unravel the mixture statistics to obtain a picture of the time evolution of the early immune system. Sequence repertoire analysis also allows us to detect the statistical impact of selection on the output of the VDJ recombination process. The effects we find are nearly identical between thymus and blood, suggesting that our analysis mainly detects selection for proper folding of the TCR receptor protein. We further find that selection is weaker in laboratory mice than in humans and it does not affect the diversity of the repertoire.

摘要

适应性免疫系统能够对任意病原体做出反应,其基础是免疫细胞表面受体的广泛多样性。这种多样性源于一种随机的 DNA 编辑过程(VDJ 重组),每当一个新的免疫细胞从干细胞中产生时,这个过程就会作用于表面受体基因。通过分析来自不同年龄的小鼠血液和胸腺中的 T 细胞受体(TCR)序列库,我们量化了从胚胎到年轻成年过程中 VDJ 重组过程发生的变化。我们发现,随着年龄的增长,随机插入的数量会迅速增加,多样性也会显著增加。由于血液会随着时间的推移不断积累来自胸腺的输出,因此血液中的 TCR 序列库是不同统计重组过程的混合物,我们解开了这种混合物的统计数据,以获得早期免疫系统的时间演化图。序列库分析还使我们能够检测到选择对 VDJ 重组过程输出的统计影响。我们发现的影响在胸腺和血液之间几乎完全相同,这表明我们的分析主要检测了 TCR 受体蛋白正确折叠的选择。我们还发现,与人类相比,实验室小鼠中的选择较弱,并且不会影响 TCR 序列库的多样性。

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