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CD8+树突状细胞(DC)是否决细胞吗?CD8在DC发育以及CD4和CD8 T细胞反应调节中对DC的作用。

Are CD8+ dendritic cells (DC) veto cells? The role of CD8 on DC in DC development and in the regulation of CD4 and CD8 T cell responses.

作者信息

Kronin V, Vremec D, Winkel K, Classon B J, Miller R G, Mak T W, Shortman K, Süss G

机构信息

Walter and Eliza Hall Institute of Medical Research, Melbourne, Victoria, Australia.

出版信息

Int Immunol. 1997 Jul;9(7):1061-4. doi: 10.1093/intimm/9.7.1061.

DOI:10.1093/intimm/9.7.1061
PMID:9237115
Abstract

The CD8-expressing dendritic cells (DC) present in mouse spleen have been shown to have a regulatory effect on the CD4 and CD8 T cells they activate, restricting subsequent T cell proliferation by either inducing apoptotic T cell death (CD4 T cells) or by limiting endogenous cytokine production (CD8 T cells). To determine the role of the CD8 molecule itself in these regulatory phenomena, the DC from CD8 null mice were studied. The DC marker DEC-205 (NLDC 145) was used as a surrogate marker for CD8, since the expression of these two molecules on splenic DC was closely correlated. DC levels were normal, and the incidence of DEC-205+ and DEC-205- DC was normal in CD8 null mice, indicating that the absence of CD8 did not affect DC development. The proliferative response of T cells to allogeneic DEC-205+ DC from either CD8-/- or CD8+/+ mice was similar and was much less than the response to DEC-205- DC from these mice. This applied to both the CD4 and the CD8 T cell responses. Thus the lack of the CD8 molecule did not affect the stimulatory or regulatory properties of the DC. The regulatory CD8+ DEC-205+ DC therefore differ in that respect from antigen-presenting 'veto' cells, where CD8 itself is involved in transmitting negative signals to the T cells. DEC-205 may prove to be a more pertinent marker of the regulatory DC population.

摘要

已证明存在于小鼠脾脏中的表达CD8的树突状细胞(DC)对其激活的CD4和CD8 T细胞具有调节作用,通过诱导凋亡性T细胞死亡(CD4 T细胞)或限制内源性细胞因子产生(CD8 T细胞)来限制随后的T细胞增殖。为了确定CD8分子本身在这些调节现象中的作用,对来自CD8基因敲除小鼠的DC进行了研究。DC标志物DEC-205(NLDC 145)被用作CD8的替代标志物,因为这两种分子在脾脏DC上的表达密切相关。CD8基因敲除小鼠的DC水平正常,DEC-205+和DEC-205- DC的发生率也正常,这表明CD8的缺失不影响DC的发育。T细胞对来自CD8-/-或CD8+/+小鼠的同种异体DEC-205+ DC的增殖反应相似,且远低于对这些小鼠的DEC-205- DC的反应。这适用于CD4和CD8 T细胞反应。因此,CD8分子的缺失不影响DC的刺激或调节特性。因此,调节性CD8+ DEC-205+ DC在这方面与抗原呈递“否决”细胞不同,在“否决”细胞中,CD8本身参与向T细胞传递负信号。DEC-205可能被证明是调节性DC群体更相关的标志物。

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