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健康人群中CD4和CD8 T细胞亚群随年龄的动态表型重塑:一种分区模型分析

Dynamic phenotypic restructuring of the CD4 and CD8 T-cell subsets with age in healthy humans: a compartmental model analysis.

作者信息

Jackola D R, Hallgren H M

机构信息

Department of Medicine, University of Minnesota Medical School, Minneapolis 55455, USA.

出版信息

Mech Ageing Dev. 1998 Nov 16;105(3):241-64. doi: 10.1016/s0047-6374(98)00089-x.

DOI:10.1016/s0047-6374(98)00089-x
PMID:9862233
Abstract

In healthy humans, phenotypic restructuring occurs with age within the CD3+ T-lymphocyte complement. This is characterized by a non-linear decrease of the percentage of 'naive' (CD45RA+) cells and a corresponding non-linear increase of the percentage of 'memory' (CD45R0+) cells among both the CD4+ and CD8+ T-cell subsets. We devised a simple compartmental model to study the age-dependent kinetics of phenotypic restructuring. We also derived differential equations whose parameters determined yearly gains minus losses of the percentage and absolute numbers of circulating naive cells, yearly gains minus losses of the percentage and absolute numbers of circulating memory cells, and the yearly rate of conversion of naive to memory cells. Solutions of these evaluative differential equations demonstrate the following: (1) the memory cell complement 'resides' within its compartment for a longer time than the naive cell complement within its compartment for both CD4 and CD8 cells; (2) the average, annual 'turnover rate' is the same for CD4 and CD8 naive cells. In contrast, the average, annual 'turnover rate' for memory CD8 cells is 1.5 times that of memory CD4 cells; (3) the average, annual conversion rate of CD4 naive cells to memory cells is twice that of the CD8 conversion rate; (4) a transition in dynamic restructuring occurs during the third decade of life that is due to these differences in turnover and conversion rates, between and from naive to memory cells.

摘要

在健康人体内,CD3 + T淋巴细胞补体随年龄发生表型重构。其特征是,在CD4 +和CD8 + T细胞亚群中,“初始”(CD45RA +)细胞百分比呈非线性下降,相应地,“记忆”(CD45R0 +)细胞百分比呈非线性增加。我们设计了一个简单的区室模型来研究表型重构的年龄依赖性动力学。我们还推导了微分方程,其参数决定了循环初始细胞百分比和绝对数量的年增加量减去年减少量、循环记忆细胞百分比和绝对数量的年增加量减去年减少量,以及初始细胞向记忆细胞转化的年速率。这些评估性微分方程的解表明:(1)对于CD4和CD8细胞,记忆细胞补体在其区室内的“驻留”时间比初始细胞补体在其区室内的时间更长;(2)CD4和CD8初始细胞的平均年“周转率”相同。相比之下,记忆CD8细胞的平均年“周转率”是记忆CD4细胞的1.5倍;(3)CD4初始细胞向记忆细胞的平均年转化率是CD8转化率的两倍;(4)由于初始细胞与记忆细胞之间以及从初始细胞向记忆细胞转化的周转率差异,在生命的第三个十年会发生动态重构的转变。

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