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人类效应性CD4 T细胞功能的近端信号传导控制

Proximal signaling control of human effector CD4 T cell function.

作者信息

Okoye Francesca I, Krishnan Sandeep, Chandok Meena R, Tsokos George C, Farber Donna L

机构信息

Division of Transplantation, Department of Surgery, University of Maryland School of Medicine, MSTF Building, Room 400, Baltimore, MD 21201, USA.

出版信息

Clin Immunol. 2007 Oct;125(1):5-15. doi: 10.1016/j.clim.2007.07.002. Epub 2007 Aug 9.

Abstract

The functional coupling of T cell receptor (TCR)-mediated signaling events in primary human T cells remains undefined. We demonstrate here that alterations in the expression of proximal TCR-coupled signaling subunits are associated with distinct effector capacities in differentiated human CD4 T cells. Analysis of proximal signaling profiles using biochemical and single cell approaches reveals decreased CD3zeta and ZAP-70 expression correlating with functional anergy, with increased CD3zeta/ ZAP-70 expression and phosphorylation connoting acquisition of effector capacity. By contrast, the FcRgamma signaling subunit known to be expressed in human effector cells and in T cells from the autoimmune disease SLE is up-regulated upon activation, yet does not correlate with functional capacity in effector cells, and does not alter signaling or function in primary FcRgamma transfectants. Our results have implications for targeting signaling molecules in immunotherapy and evaluating the functional consequence of signaling alterations associated with autoimmunity and chronic diseases.

摘要

人原代T细胞中T细胞受体(TCR)介导的信号事件的功能偶联仍不明确。我们在此证明,近端TCR偶联信号亚基表达的改变与分化的人CD4 T细胞中不同的效应能力相关。使用生化和单细胞方法分析近端信号谱显示,CD3ζ和ZAP-70表达降低与功能无能相关,而CD3ζ/ZAP-70表达和磷酸化增加意味着效应能力的获得。相比之下,已知在人类效应细胞和自身免疫性疾病SLE的T细胞中表达的FcRγ信号亚基在激活后上调,但与效应细胞的功能能力无关,并且不会改变原代FcRγ转染细胞中的信号传导或功能。我们的结果对于免疫治疗中靶向信号分子以及评估与自身免疫和慢性疾病相关的信号改变的功能后果具有启示意义。

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