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首页> 外文期刊>The Journal of Immunology: Official Journal of the American Association of Immunologists >Endocytosis of Cytotoxic Granules Is Essential for Multiple Killing of Target Cells by T Lymphocytes
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Endocytosis of Cytotoxic Granules Is Essential for Multiple Killing of Target Cells by T Lymphocytes

机译:细胞毒性颗粒的内吞作用对于T淋巴细胞多次杀死靶细胞至关重要

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摘要

CTLs are serial killers that kill multiple target cells via exocytosis of cytotoxic granules (CGs). CG exocytosis is tightly regulated and has been investigated in great detail; however, whether CG proteins are endocytosed following exocytosis and contribute to serial killing remains unknown. By using primary CTLs derived from a knock-in mouse of the CG membrane protein Synaptobrevin2, we show that CGs are endocytosed in a clathrin-and dynamin-dependent manner. Following acidification, endocytosed CGs are recycled through early and late, but not recycling endosomes. CGs are refilled with granzyme B at the late endosome stage and polarize to subsequent synapses formed between the CTL and new target cells. Importantly, inhibiting CG endocytosis in CTLs results in a significant reduction of their cytotoxic activity. Thus, our data demonstrate that continuous endocytosis of CG membrane proteins is a prerequisite for efficient serial killing of CTLs and identify key events in this process.
机译:CTL是通过细胞毒性颗粒(CGs)的胞吐作用杀死多个靶细胞的系列杀手。 CG的胞吐作用受到严格的调控,已经进行了详细的研究。然而,CG蛋白是否在胞吐作用后被内吞并导致连续杀伤尚不清楚。通过使用源于CG膜蛋白Synaptobrevin2的敲入小鼠的初级CTL,我们显示CGs以网格蛋白和动力蛋白依赖性方式被内吞。酸化后,内吞的CGs可以通过早期和晚期循环利用,而不能循环利用内体。 CG在核内体晚期被粒酶B充满,并极化至CTL和新靶细胞之间形成的后续突触。重要的是,抑制CTL中的CG内吞作用会导致其细胞毒性活性显着降低。因此,我们的数据表明,CG膜蛋白的连续内吞作用是有效连续杀伤CTL并确定此过程中关键事件的先决条件。

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