Human fetal T cells: Insights into developmental specialization and mechanisms of lineage transition

IF 7.5 2区医学 Q1 IMMUNOLOGY

Immunological Reviews Pub Date : 2023-03-24 DOI:10.1111/imr.13195

Trevor D. Burt, Joseph M. McCune

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引用次数: 1

Abstract

The switch from primitive to definitive hematopoiesis occurs early in development through the emergence of a wave of definitive hematopoietic stem cells from intraembryonic sites, supplanting the original primitive population of extraembryonically derived stem cells. When it became clear that unique features of the fetal immune system could not be reproduced by adult stem cells, it was hypothesized that a lineage of definitive fetal hematopoietic stem cells predominates antenatally, ultimately giving way to an emerging wave of adult stem cells and resulting in a “layered” fetal immune system consisting of overlapping lineages. It is now clear, however, that the transition from human fetal-to-adult T cell identity and function does not occur due to a binary switch between distinct fetal and adult lineages. Rather, recent evidence from single cell analysis suggests that during the latter half of fetal development a gradual, progressive transition occurs at the level of hematopoietic stem-progenitor cells (HSPCs) which is reflected in their T cell progeny. At a transcriptional level, clusters of genes are up- and down-regulated with sequenced timing, suggesting that the transition is under the control of master regulatory factors, including epigenetic modifiers. The net effect is still one of “molecular layering,” that is, the continuous layering of iterative generations of HSPCs and T cells that arise through progressive changes in gene expression. This review will focus on recent discoveries that elucidate mechanisms of fetal T cell function and the transition from fetal to adult identity. The epigenetic landscape of fetal T cells facilitates their ability to fulfill the dominant fetal mandate of generating tolerance against self, maternal, and environmental antigens by supporting their predisposition to differentiate into CD25⁺FoxP3⁺ regulatory T cells (T_Regs). We will explore how the coordinated development of two complementary populations of fetal T cells—conventional T cells dominated by T_Regs and tissue-associated memory effector cells with innate-like inflammatory potential—is crucial not only for maintaining intrauterine immune quiescence but also for facilitating an immune response that is appropriately tuned for the bombardment of antigen stimulation that happens at birth.

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人类胎儿T细胞:对发育特化和谱系转变机制的见解

从原始造血到最终造血的转变发生在发育早期，通过胚胎内位置出现的一波最终造血干细胞，取代原始的胚外来源的干细胞群。当很明显胎儿免疫系统的独特特征不能被成体干细胞复制时，人们假设胎儿造血干细胞的谱系在产前占主导地位，最终让位于新兴的成体干细胞，并导致由重叠谱系组成的“分层”胎儿免疫系统。然而，现在很清楚的是，从胎儿到成人的T细胞身份和功能的转变并不是因为不同胎儿和成人谱系之间的二元切换而发生的。相反，最近来自单细胞分析的证据表明，在胎儿发育的后半期，造血干细胞(HSPCs)水平发生了渐进的转变，这反映在它们的T细胞后代中。在转录水平上，基因簇随着测序时间的变化而上调和下调，这表明这种转变是在包括表观遗传修饰因子在内的主调控因子的控制下进行的。净效应仍然是“分子分层”之一，即通过基因表达的渐进式变化产生的HSPCs和T细胞的迭代代的连续分层。这篇综述将集中在最近的发现阐明胎儿T细胞功能的机制和从胎儿到成人身份的转变。胎儿T细胞的表观遗传环境通过支持它们向CD25+FoxP3+调节性T细胞(TRegs)分化的倾向，促进了它们完成对自身、母体和环境抗原产生耐受性的主要胎儿任务的能力。我们将探讨两种互补的胎儿T细胞群——由TRegs主导的传统T细胞和具有先天炎性潜能的组织相关记忆效应细胞——如何协调发展，这不仅对维持宫内免疫静止至关重要，而且对促进免疫反应至关重要，这种免疫反应可以适当地调节出生时发生的抗原刺激轰击。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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来源期刊

Immunological Reviews 医学-免疫学

CiteScore

16.20

自引率

1.10%

发文量

118

审稿时长

4-8 weeks

期刊介绍： Immunological Reviews is a specialized journal that focuses on various aspects of immunological research. It encompasses a wide range of topics, such as clinical immunology, experimental immunology, and investigations related to allergy and the immune system. The journal follows a unique approach where each volume is dedicated solely to a specific area of immunological research. However, collectively, these volumes aim to offer an extensive and up-to-date overview of the latest advancements in basic immunology and their practical implications in clinical settings.