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首页> 外文期刊>The Journal of Immunology: Official Journal of the American Association of Immunologists >Docking of lytic granules at the immunological synapse in human CTL requires Vti1b-dependent pairing with CD3 endosomes.
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Docking of lytic granules at the immunological synapse in human CTL requires Vti1b-dependent pairing with CD3 endosomes.

机译:在人类CTL的免疫突触中对接裂解颗粒需要Vti1b依赖性与CD3内体的配对。

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摘要

Lytic granule (LG)-mediated apoptosis is the main mechanism by which CTL kill virus-infected and tumorigenic target cells. CTL form a tight junction with the target cells, which is called the immunological synapse (IS). To avoid unwanted killing of neighboring cells, exocytosis of lytic granules (LG) is tightly controlled and restricted to the IS. In this study, we show that in activated human primary CD8(+) T cells, docking of LG at the IS requires tethering LG with CD3-containing endosomes (CD3-endo). Combining total internal reflection fluorescence microscopy and fast deconvolution microscopy (both in living cells) with confocal microscopy (in fixed cells), we found that LG and CD3-endo tether and are cotransported to the IS. Paired but not single LG are accumulated at the IS. The dwell time of LG at the IS is substantially enhanced by tethering with CD3-endo, resulting in a preferential release of paired LG over single LG. The SNARE protein Vti1b is required for tethering of LG and CD3-endo. Downregulation of Vti1b reduces tethering of LG with CD3-endo. This leads to an impaired accumulation and docking of LG at the IS and a reduction of target cell killing. Therefore, Vti1b-dependent tethering of LG and CD3-endo determines accumulation, docking, and efficient lytic granule secretion at the IS.
机译:溶胞颗粒(LG)介导的凋亡是CTL杀死病毒感染和致瘤靶细胞的主要机制。 CTL与靶细胞形成紧密连接,称为免疫突触(IS)。为了避免不必要地杀死邻近细胞,溶胞颗粒(LG)的胞吐作用受到严格控制,并仅限于IS。在这项研究中,我们表明,在激活的人类原代CD8(+)T细胞中,LG在IS处的对接需要将LG与包含CD3的内体(CD3-Endo)捆绑在一起。将全内反射荧光显微镜和快速反卷积显微镜(均在活细胞中)与共聚焦显微镜(在固定细胞中)相结合,我们发现LG和CD3内在系链并共转运至IS。配对但不是单个LG会在IS上累积。通过与CD3-endo绑定,可以大大提高LG在IS上的停留时间,从而导致配对LG优先于单个LG释放。 SNARE蛋白Vti1b是LG与CD3-endo的系结所必需的。 Vti1b的下调减少了LG与CD3-endo的束缚。这导致LG在IS处的积累和对接受损,并降低了靶细胞的杀伤力。因此,LG和CD3-endo的Vti1b依赖型系链决定了IS处的积累,对接和有效的溶解性颗粒分泌。

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