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首页> 外文期刊>The Journal of Immunology: Official Journal of the American Association of Immunologists >CD154/CD40 and CD70/CD27 interactions have different and sequential functions in T cell-dependent B cell responses: enhancement of plasma cell differentiation by CD27 signaling.
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CD154/CD40 and CD70/CD27 interactions have different and sequential functions in T cell-dependent B cell responses: enhancement of plasma cell differentiation by CD27 signaling.

机译:CD154 / CD40和CD70 / CD27相互作用在依赖T细胞的B细胞反应中具有不同的顺序功能:通过CD27信号传导增强浆细胞分化。

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摘要

CD40, a TNF receptor family member, plays a central role in T cell-mediated B cell activation. We have recently demonstrated that CD27, another TNF receptor family member, was also involved in B cell regulation and enhanced Ig production. In this report we compare CD27 and CD40 signals in B cell function. We selectively mimicked the effect of T cell help by addition to peripheral blood B cells activated with Staphylococcus aureus Cowan I strain and IL-2 of irradiated 300-19 cells transfected with either the CD70 (CD27 ligand) gene or the CD154 (CD40 ligand) gene, the vector alone, or both CD70 and CD154 genes. CD27 ligation induced only a slight increase in B cell proliferation compared with the dramatic enhancement induced by CD40 ligation; double ligation proved to be less efficient than CD40 ligation alone. In contrast, IgG production was increased only by CD27 ligation alone. Moreover, the CD27 signal was more efficient when it was given on day 2 of the culture rather than on day 0. Phenotypic analysis of the activated cells showed that CD27 ligation increased the percentage of cells showing a plasma cell profile (CD19-, CD38+), whereas upon CD40 ligation most of the cells still had a germinal center-like phenotype (CD19+, CD38+). Our results suggest that the CD27 and CD40 signals are not synergistic but, rather, are complementary and involve distinct steps of T cell-dependent B cell activation. CD27 may be more important in the induction of plasma cell differentiation at a time when the expansion phase has already occurred.
机译:TNF受体家族成员CD40在T细胞介导的B细胞活化中起着核心作用。我们最近证明,另一种TNF受体家族成员CD27也参与了B细胞的调节和Ig的产生。在这份报告中,我们比较了B细胞功能中的CD27和CD40信号。通过选择性地模仿金黄色葡萄球菌Cowan I株激活的外周血B细胞和用CD70(CD27配体)基因或CD154(CD40配体)转染的300-19细胞的IL-2激活,可以选择性地模拟T细胞的帮助作用。基因,单独的载体或CD70和CD154基因。与CD40连接引起的显着增强相比,CD27连接仅诱导B细胞增殖略有增加;事实证明,双重连接比单独的CD40连接效率低。相反,仅通过CD27连接可增加IgG的产生。此外,在培养的第2天而不是第0天给予CD27信号时,效率更高。对活化细胞的表型分析表明,CD27连接增加了显示浆细胞谱的细胞百分比(CD19-,CD38 +) ,而在CD40连接后,大多数细胞仍具有生发中心样表型(CD19 +,CD38 +)。我们的结果表明,CD27和CD40信号不是协同作用,而是互补的,并且涉及T细胞依赖性B细胞活化的不同步骤。在已经发生扩张阶段的时候,CD27在诱导浆细胞分化中可能更为重要。

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