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首页> 外文期刊>Immunological reviews. >Compartmentalization of signaling by vesicular trafficking: a shared building design for the immune synapse and the primary cilium.
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Compartmentalization of signaling by vesicular trafficking: a shared building design for the immune synapse and the primary cilium.

机译:囊泡运输信号传导的区室化:免疫突触和初级纤毛的共享建筑设计。

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摘要

Accumulating evidence underscores the immune synapse (IS) of naive T cells as a site of intense vesicular trafficking. At variance with helper and cytolytic effectors, which use the IS as a secretory platform to deliver cytokines and/or lytic granules to their cellular targets, this process is exploited by naive T cells as a means to regulate the assembly and maintenance of the IS, on which productive signaling and cell activation crucially depend. We have recently identified a role of the intraflagellar transport (IFT) system, which is responsible for the assembly of the primary cilium, in the non-ciliated T-cell, where it controls IS assembly by promoting polarized T-cell receptor recycling. This unexpected finding not only provides new insight into the mechanisms of IS assembly but also strongly supports the notion that the IS and the primary cilium, which are both characterized by a specialized membrane domain highly enriched in receptors and signaling mediators, share architectural similarities and are homologous structures. Here, we review our current understanding of vesicular trafficking in the regulation of the assembly and maintenance of the naive T-cell IS and the primary cilium, with a focus on the IFT system.
机译:越来越多的证据强调,幼稚T细胞的免疫突触(IS)是强烈的囊泡运输部位。与使用IS作为分泌平台将细胞因子和/或裂解颗粒传递至其细胞靶标的辅助和细胞溶解效应子有所不同,幼稚T细胞利用这一过程来调节IS的组装和维持,生产信号和细胞活化主要取决于哪一个。我们最近确定了鞭毛内运输(IFT)系统的作用,该系统负责非纤毛T细胞中初级纤毛的组装,并通过促进极化T细胞受体的再循环来控制IS组装。这一出乎意料的发现不仅提供了对IS组装机制的新见解,而且还强烈支持以下观点:IS和初级纤毛均以高度富集受体和信号介体的专门膜结构域为特征,具有相似的结构并在同源结构。在这里,我们回顾我们对水泡运输的当前理解,主要是对IFT系统进行研究,以了解幼稚T细胞IS和初级纤毛的组装和维持情况。

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