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源自外周血的CD4+CD57+ T细胞不支持B细胞产生免疫球蛋白。

CD4+CD57+ T cells derived from peripheral blood do not support immunoglobulin production by B cells.

作者信息

Andersson E, Ohlin M, Borrebaeck C A, Carlsson R

机构信息

Department of Immunotechnology, Lund University, Sweden.

出版信息

Cell Immunol. 1995 Jul;163(2):245-53. doi: 10.1006/cimm.1995.1123.

Abstract

A small subpopulation of CD4+ T cells found in peripheral blood coexpresses the CD57+ marker normally found on, e.g., NK cells. It is known that this population occurs in a higher frequency in certain diseases. The same antigen has also been shown to be expressed on CD4+ T cells derived from germinal centers. The localization of this cell population to specialized lymphoid structures suggests that it may play a role in the evolution of the antibody response following antigenic stimulation in vivo. We have examined the ability of peripheral blood helper T cells coexpressing CD57 to participate in B cell activation/differentiation and evaluated their responses to polyclonal stimulation. The CD4+CD57+ T cells do not express mRNA for a number of different cytokines or for the CD40 ligand after activation in vitro. Furthermore these cells do not induce differentiation of B cells into immunoglobulin-producing cells. Consequently, despite their CD4 phenotype and their ability to be activated, to express the IL-2 receptor, and to enter into the cell cycle, they do not act as T helper cells under conditions where CD4+/CD57- cells normally do so. The findings suggest that this peripheral blood helper T cell population is functionally different from regular CD4+ T cells. The basis for the lack of proper costimulatory signals for immunoglobulin production might be related to the low expression of CD28.

摘要

在外周血中发现的一小部分CD4+ T细胞共表达通常在例如自然杀伤细胞(NK细胞)上发现的CD57+标志物。已知该细胞群在某些疾病中出现的频率更高。同样的抗原也已被证明在生发中心来源的CD4+ T细胞上表达。该细胞群定位于特殊的淋巴结构表明它可能在体内抗原刺激后抗体反应的演变中发挥作用。我们已经检测了共表达CD57的外周血辅助性T细胞参与B细胞活化/分化的能力,并评估了它们对多克隆刺激的反应。体外激活后,CD4+CD57+ T细胞不表达多种不同细胞因子或CD40配体的mRNA。此外,这些细胞不会诱导B细胞分化为产生免疫球蛋白的细胞。因此,尽管它们具有CD4表型,并且能够被激活、表达IL-2受体并进入细胞周期,但在CD4+/CD57-细胞通常发挥作用的条件下,它们并不作为辅助性T细胞发挥作用。这些发现表明,这群外周血辅助性T细胞在功能上与常规CD4+ T细胞不同。缺乏产生免疫球蛋白的适当共刺激信号的基础可能与CD28的低表达有关。

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