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信号淋巴细胞激活分子在CD40配体激活的树突状细胞上表达,并直接增强炎性细胞因子的产生。

Signaling lymphocytic activation molecule is expressed on CD40 ligand-activated dendritic cells and directly augments production of inflammatory cytokines.

作者信息

Bleharski J R, Niazi K R, Sieling P A, Cheng G, Modlin R L

机构信息

Department of Medicine, Division of Dermatology, Jonsson Comprehensive Cancer Center, and Molecular Biology Institute, University of California School of Medicine, Los Angeles, CA 90095, USA.

出版信息

J Immunol. 2001 Sep 15;167(6):3174-81. doi: 10.4049/jimmunol.167.6.3174.

Abstract

Dendritic cells (DC) comprise a key part of the innate immune system that, upon activation, profoundly influences the nature of the adaptive T cell response. In this study, we present evidence that signaling lymphocytic activation molecule (SLAM), a molecule first identified in activated T and B cells, is strongly up-regulated in DC activated through CD40, as well as in response to inflammatory stimuli, including polyinosinic polycytidylic acid and LPS. mRNA encoding both membrane-bound and soluble secreted isoforms of SLAM was detected in CD40 ligand-activated DC, comprising two of the four known SLAM isoforms. Expression of membrane-bound SLAM protein peaked at 12 h poststimulation with CD40 ligand, gradually returning to baseline levels after 6 days. SLAM up-regulation appears to be a direct result of the induction of DC maturation, as inflammatory cytokines released during this process do not affect SLAM expression. Functionally, engagement of SLAM enhances DC production of IL-12 and IL-8, while having no effect on production of IL-10. Because SLAM is involved in the activation of T cells, the expression of SLAM on DC may provide a bidirectional signaling mechanism in which interacting DC and T cells are simultaneously and synergistically activated to mount proinflammatory Th1 responses.

摘要

树突状细胞(DC)是先天性免疫系统的关键组成部分,一旦被激活,会深刻影响适应性T细胞反应的性质。在本研究中,我们提供证据表明,信号淋巴细胞激活分子(SLAM),一种最初在活化的T细胞和B细胞中发现的分子,在通过CD40激活的DC中以及对包括多聚肌苷酸胞苷酸和脂多糖在内的炎症刺激反应中强烈上调。在CD40配体激活的DC中检测到编码膜结合和可溶性分泌型SLAM亚型的mRNA,这是四种已知SLAM亚型中的两种。膜结合型SLAM蛋白的表达在CD40配体刺激后12小时达到峰值,6天后逐渐恢复到基线水平。SLAM上调似乎是DC成熟诱导的直接结果,因为在此过程中释放的炎症细胞因子不影响SLAM表达。在功能上,SLAM的结合增强了DC产生IL-12和IL-8的能力,而对IL-10的产生没有影响。由于SLAM参与T细胞的激活,DC上SLAM的表达可能提供一种双向信号传导机制 在这种机制中,相互作用的DC和T细胞同时被协同激活,以引发促炎性Th1反应。

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