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效应T淋巴细胞中钙信号的奇点

Singularities of calcium signaling in effector T-lymphocytes.

作者信息

Robert Virginie, Triffaux Emily, Savignac Magali, Pelletier Lucette

机构信息

INSERM U1043, Toulouse, F-31024, France.

出版信息

Biochim Biophys Acta. 2013 Jul;1833(7):1595-602. doi: 10.1016/j.bbamcr.2012.12.001. Epub 2012 Dec 20.

DOI:10.1016/j.bbamcr.2012.12.001
PMID:23266355
Abstract

CD4(+) helper T (Th) lymphocytes orchestrate the immune response and include several types of effectors such as Th1, Th17 and Th2 cells. They fight against intracellular, extracellular pathogens and parasites respectively. They may also cause distinct immunopathological disorders. Th1 and Th17 are implicated in the development of autoimmune diseases while Th2 cells can initiate allergic diseases. These subsets differ by their TCR-associated signaling. In addition, the regulation of intracellular calcium concentration is not the same in Th1, Th2 and 17 cells. Our group showed that Th2 cells selectively overexpressed voltage-activated calcium (Cav1)-related channels. An increasing number of groups report the presence of Cav1-related products in T-lymphocyte subsets. This is a matter of debate since these calcium channels are classically defined as activated by high cell membrane depolarization in excitable cells. However, the use of mice with ablation of some Cav1 subunits shows undoubtedly an immune phenotype raising the question of how Cav1 channels are regulated in lymphocytes. We showed that knocking down Cav1.2 and/or Cav1.3 subunits impairs the functions of Th2 lymphocytes and is beneficial in experimental models of asthma, while it has no effect on Th1 cell functions. Beyond the role of Cav1 channels in T-lymphocytes, the identification of key components selectively implicated in one or the other T cell subset paves the way for the design of new selective therapeutic targets in the treatment of immune disorders while preserving the other T-cell subsets. This article is part of a Special Issue entitled: 12th European Symposium on Calcium.

摘要

CD4(+)辅助性T(Th)淋巴细胞协调免疫反应,包括几种效应细胞类型,如Th1、Th17和Th2细胞。它们分别对抗细胞内、细胞外病原体和寄生虫。它们也可能导致不同的免疫病理紊乱。Th1和Th17与自身免疫性疾病的发展有关,而Th2细胞可引发过敏性疾病。这些亚群因其与TCR相关的信号传导而有所不同。此外,Th1、Th2和Th17细胞内钙浓度的调节也不相同。我们的研究小组表明,Th2细胞选择性地过度表达电压激活钙(Cav1)相关通道。越来越多的研究小组报道在T淋巴细胞亚群中存在Cav1相关产物。这是一个有争议的问题,因为这些钙通道传统上被定义为在可兴奋细胞中由高细胞膜去极化激活。然而,使用敲除某些Cav1亚基的小鼠无疑显示出一种免疫表型,这就提出了Cav1通道在淋巴细胞中如何被调节的问题。我们表明,敲低Cav1.2和/或Cav1.3亚基会损害Th2淋巴细胞的功能,在哮喘实验模型中是有益的,而对Th1细胞功能没有影响。除了Cav1通道在T淋巴细胞中的作用外,鉴定选择性地与一种或另一种T细胞亚群相关的关键成分,为设计治疗免疫紊乱的新的选择性治疗靶点铺平了道路,同时保留其他T细胞亚群。本文是名为:第12届欧洲钙研讨会的特刊的一部分。

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