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首页> 外文期刊>The Journal of Immunology: Official Journal of the American Association of Immunologists >Reevaluation of T cell receptor excision circles as a measure of human recent thymic emigrants.
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Reevaluation of T cell receptor excision circles as a measure of human recent thymic emigrants.

机译:重新评估T细胞受体切除环作为人类近期胸腺迁徙的一种度量。

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摘要

The human thymus exports newly generated T cells to the periphery. As no markers have been identified for these recent thymic emigrants (RTE), it is presently impossible to measure human thymic output. T cell receptor excision circles (TREC) have been recently used to assess thymic output during both health and disease. Using a mathematical model, we quantify age-dependent changes both in the number of RTE generated per day and in TREC concentration during an 80-year lifespan. Through analyses, we demonstrate that RTE and peripheral T cell division have the same potential to affect TREC concentration at any age in healthy people. T cell death also influences TREC concentration, but to a lesser extent. During aging, our results indicate that thymic involution primarily induces an age-dependent decline in TREC concentrations within both CD4(+) and CD8(+) T cell populations. We further apply this model for studying TREC concentration during HIV-1 infection. Our analyses reveal that a decrease in thymic output is the major contributor to the decline in TREC concentration within CD4(+) T cells, whereas both increased peripheral T cell division and decreased thymic output induce the decline in TREC concentration within CD8(+) T cells. Therefore, we suggest that T cell turnover should be examined together with TREC concentration as a measure of RTE. If peripheral T cell division remains relatively unchanged, then TREC concentration indeed reflects thymic output.
机译:人胸腺将新产生的T细胞输出到周围。由于尚未为这些最近的胸腺迁徙者(RTE)鉴定出任何标记,因此目前无法测量人的胸腺输出量。 T细胞受体切除环(TREC)最近已用于评估健康和疾病期间的胸腺输出量。使用数学模型,我们可以量化80年寿命期间每天产生的RTE数量和TREC浓度的年龄相关变化。通过分析,我们证明了健康人在任何年龄段,RTE和外周T细胞分裂都具有相同的潜力来影响TREC浓度。 T细胞死亡也影响TREC浓度,但程度较小。在衰老过程中,我们的结果表明,胸腺退化主要诱导CD4(+)和CD8(+)T细胞群体中TREC浓度的年龄依赖性下降。我们进一步将该模型用于研究HIV-1感染期间的TREC浓度。我们的分析表明,胸腺输出的减少是CD4(+)T细胞内TREC浓度下降的主要原因,而外周T细胞分裂增加和胸腺输出减少均引起CD8(+)T内TREC浓度下降。细胞。因此,我们建议应将T细胞周转率与TREC浓度一起检查以衡量RTE。如果外周T细胞分裂保持相对不变,则TREC浓度确实反映了胸腺输出。

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