由CD45异构体表达所定义的CD8 + T细胞亚群在产生白细胞介素-2、γ干扰素和肿瘤坏死因子-β的能力上存在差异。

CD8+ T-cell subsets defined by expression of CD45 isoforms differ in their capacity to produce IL-2, IFN-gamma and TNF-beta.

作者信息

Adamthwaite D, Cooley M A

机构信息

Centre for Immunology, St Vincent's Hospital, Darlinghurst, NSW, Australia.

出版信息

Immunology. 1994 Feb;81(2):253-60.

PMID:7908892

原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC1422313/

Abstract

Expression of different isoforms of CD45, the leucocyte common antigen (LCA), on T-cell subsets has permitted distinctions between the functional activities of subpopulations within the major CD4+ T-cell subset. With respect to cytokine production, the expression on CD4+ cells of CD45RA, a high molecular weight isoform, defines a population which produces only interleukin-2 (IL-2) and tumour necrosis factor-beta (TNF-beta) in quantity, with peak production of IL-2 occurring after 24-48 hr stimulation, while the CD4+ population bearing high levels of CD45RO, a low molecular weight isoform, can produce a wide range of cytokines within 24 hr of activation. The literature is conflicting on the capacities for cytokine production of CD8+ subsets divided on the basis of either CD45RA or CD45RO expression. The aim of this study was to attempt to clarify this area by determining the amount and kinetics of production of IL-2, interferon-gamma (IFN-gamma) and TNF-beta in CD8+ cells separated on the basis of both CD45RA and CD45RO isoform expression. The results showed that CD8+ CD45RA- and CD8+ CD45RO+ T lymphocytes produce significantly more of all three cytokines than do CD8+ CD45RA+ or CD8+ CD45RO- T cells. The kinetics for IFN-gamma and TNF-beta production were similar for both subsets, while IL-2 production was delayed by approximately 3 hr in the CD8+ CD45RO- population as compared to the CD8+ CD45RO+ subset. It is suggested that some of the confusion over cytokine production by these CD8+ subsets may be attributable to different conditions for isolation causing pre-activation of positively selected populations. It is also suggested that while CD8+ CD45RA+ cells are shown to acquire CD45RO upon activation, as do CD4+ CD45RA+ cells, the results of the present study argue for a different relationship between CD8+ subsets separated on the basis of CD45 isoform expression than between the corresponding CD4+ subsets.

摘要

白细胞共同抗原（LCA）CD45不同异构体在T细胞亚群上的表达，使得区分主要CD4+ T细胞亚群内各亚群的功能活性成为可能。就细胞因子产生而言，高分子量异构体CD45RA在CD4+细胞上的表达定义了一个仅大量产生白细胞介素-2（IL-2）和肿瘤坏死因子-β（TNF-β）的群体，IL-2在刺激24 - 48小时后产量达到峰值，而高水平表达低分子量异构体CD45RO的CD4+群体在激活后24小时内可产生多种细胞因子。关于基于CD45RA或CD45RO表达划分的CD8+亚群产生细胞因子的能力，文献中的观点相互矛盾。本研究的目的是通过确定基于CD45RA和CD45RO异构体表达分离的CD8+细胞中IL-2、干扰素-γ（IFN-γ）和TNF-β的产生量及动力学，来试图阐明这一领域。结果表明，CD8+ CD45RA-和CD8+ CD45RO+ T淋巴细胞产生这三种细胞因子的量均显著多于CD8+ CD45RA+或CD8+ CD45RO- T细胞。两个亚群中IFN-γ和TNF-β的产生动力学相似，而与CD8+ CD45RO+亚群相比，CD8+ CD45RO-群体中IL-2的产生延迟约3小时。有人认为，这些CD8+亚群在细胞因子产生方面的一些混淆可能归因于不同的分离条件导致阳性选择群体的预激活。还有人认为，虽然CD8+ CD45RA+细胞在激活时与CD4+ CD45RA+细胞一样会获得CD45RO，但本研究结果表明，基于CD45异构体表达分离的CD8+亚群之间的关系与相应的CD4+亚群之间的关系不同。