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Quo vadis? Interferon-inducible GTPases go to their target membranes via the LC3-conjugation system of autophagy

机译:quo vadis? 干扰素诱导的GTP酶通过自噬的LC3缀合系统转到它们的靶膜

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Many intracellular pathogens survive and replicate within vacuole-like structures in the cytoplasm. It has been unclear how the host immune system controls such pathogen-containing vacuoles. Interferon-inducible GTPases are dynamin-like GTPases that target the membranes of pathogen-containing vacuoles. Upon their oligomerization on the membrane, the vacuole structure disintegrates and the pathogen gets exposed to the hostile cytoplasm. What has been obscure is how the immune system detects and directs the GTPases to these pathogen shelters. Using a common protist parasite of mice, Toxoplasma gondii, we found that the LC3 conjugation system of autophagy is necessary and sufficient for targeting the interferon-inducible GTPases to membranes. We dubbedthis process Targeting by AutophaGy proteins (TAG). In canonical autophagy, the LC3 conjugation system is required to form membrane-bound autophagosomes, which encircle and deliver cytosolic materials to lysosomes for degradation. In TAG, however, the conjugation system is required to mark the membranes of pathogen-containing vacuoles with ubiquitin-like LC3 homologs, which function as molecular beacons to recruit the GTPases to their target membranes. Our data suggest that the LC3 conjugation system of autophagy plays an essential role in detecting and marking pathogen-containing vacuoles for immune effector targeting by the host immune system.
机译:许多细胞内病原体存活并复制在细胞质中的液泡状结构中。目前尚不清楚宿主免疫系统如何控制含这种病原体的液压。干扰素可诱导的GTP酶是靶向含有病原体的真空含量的膜状的发动机样GTP酶。在膜上的寡聚化后,储液结构崩解,病原体暴露于敌对细胞质。模糊的是免疫系统如何检测并将GTP酶引导到这些病原体避难所。使用小鼠的常见蛋白质寄生虫,我们发现,自噬的LC3缀合系统是必要的,并且足以使干扰素诱导的GTP酶靶向膜。我们用自噬蛋白(标签)赋予靶向该过程。在规范自噬中,LC3缀合系统需要形成膜结合的自噬体,其包围并将细胞溶质物质与溶酶体递送并递送至溶酶体。然而,在标签中,缀合系统需要用遍在蛋白样LC3同源物标记含病原体的真空胶剂的膜,其用作分子信标以将GTP酶募集到其靶膜上。我们的数据表明,自噬的LC3缀合系统在检测和标记宿主免疫系统靶向的免疫效应器靶向的含病原体液泡中起重要作用。

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