快速增殖和分化会损害生命早期记忆性 CD8+T 细胞的发育。
Rapid proliferation and differentiation impairs the development of memory CD8+ T cells in early life.
机构信息
Department of Microbiology and Immunology, Cornell University, Ithaca, NY 14853;
Department of Molecular Biology and Genetics, Cornell University, Ithaca, NY 14853; and.
出版信息
J Immunol. 2014 Jul 1;193(1):177-84. doi: 10.4049/jimmunol.1400553. Epub 2014 May 21.
Abstract
Neonates often generate incomplete immunity against intracellular pathogens, although the mechanism of this defect is poorly understood. An important question is whether the impaired development of memory CD8+ T cells in neonates is due to an immature priming environment or lymphocyte-intrinsic defects. In this article, we show that neonatal and adult CD8+ T cells adopted different fates when responding to equal amounts of stimulation in the same host. Whereas adult CD8+ T cells differentiated into a heterogeneous pool of effector and memory cells, neonatal CD8+ T cells preferentially gave rise to short-lived effector cells and exhibited a distinct gene expression profile. Surprisingly, impaired neonatal memory formation was not due to a lack of responsiveness, but instead because neonatal CD8+ T cells expanded more rapidly than adult cells and quickly became terminally differentiated. Collectively, these findings demonstrate that neonatal CD8+ T cells exhibit an imbalance in effector and memory CD8+ T cell differentiation, which impairs the formation of memory CD8+ T cells in early life.
摘要
新生儿通常对细胞内病原体产生不完全的免疫,尽管其机制尚不清楚。一个重要的问题是,新生儿记忆性 CD8+T 细胞发育受损是由于初始环境不成熟还是淋巴细胞内在缺陷。本文中,我们发现,当在同一宿主中对相同数量的刺激作出反应时,新生儿和成人 CD8+T 细胞采用了不同的命运。而成人 CD8+T 细胞分化为效应细胞和记忆细胞的异质群体,新生儿 CD8+T 细胞则优先产生寿命短的效应细胞,并表现出独特的基因表达谱。令人惊讶的是,新生儿记忆形成受损并不是因为缺乏反应性,而是因为新生儿 CD8+T 细胞比成人细胞扩增更快,并且很快就达到终末分化。总之,这些发现表明,新生儿 CD8+T 细胞表现出效应和记忆性 CD8+T 细胞分化的不平衡,这会损害生命早期记忆性 CD8+T 细胞的形成。
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