数量与概率:T 细胞受体库大小及其年龄变化对 T 细胞功能的影响。
Numbers and odds: TCR repertoire size and its age changes impacting on T cell functions.
机构信息
Laboratory of Molecular Biology and Immunology, National Institute on Aging, NIH, Baltimore, MD, USA.
出版信息
Semin Immunol. 2023 Sep;69:101810. doi: 10.1016/j.smim.2023.101810. Epub 2023 Jul 27.
Abstract
A vast array of αβ T cell receptors (TCRs) is generated during T cell development in the thymus through V(D)J recombination, which involves the rearrangement of multiple V, D, and J genes and the pairing of α and β chains. These diverse TCRs provide protection to the human body against a multitude of foreign pathogens and internal cancer cells. The entirety of TCRs present in an individual's T cells is referred to as the TCR repertoire. Despite an estimated 4 × 10 T cells in the adult human body, the lower bound estimate for the TCR repertoire is 3.8 × 10. While the number of circulating T cells may slightly decrease with age, the changes in the diversity of the TCR repertoire is more apparent. Here, I review recent advancements in TCR repertoire studies, the methods used to measure it, how richness and diversity change as humans age, and some of the known consequences associated with these changes.
摘要
在胸腺中,T 细胞发育过程中通过 V(D)J 重组产生了大量的 αβ T 细胞受体 (TCR),其中涉及多个 V、D 和 J 基因的重排以及 α 和 β 链的配对。这些多样化的 TCR 为人体提供了对多种外来病原体和内部癌细胞的保护。个体 T 细胞中存在的全部 TCR 被称为 TCR 库。尽管成人身体中估计有 4×10 的 T 细胞,但 TCR 库的下限估计值为 3.8×10。虽然循环 T 细胞的数量可能随年龄略有下降,但 TCR 库多样性的变化更为明显。在这里,我回顾了 TCR 库研究的最新进展、用于测量它的方法、随着人类年龄的增长丰度和多样性如何变化,以及与这些变化相关的一些已知后果。
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