Divangahi Maziar, Chen Minjian, Gan Huixian, Desjardins Danielle, Hickman Tyler T, Lee David M, Fortune Sarah, Behar Samuel M, Remold Heinz G
Department of Medicine, Brigham and Women's Hospital, Harvard Medical School, Boston, Massachusetts, USA.
Nat Immunol. 2009 Aug;10(8):899-906. doi: 10.1038/ni.1758. Epub 2009 Jun 28.
Induction of macrophage necrosis is a strategy used by virulent Mycobacterium tuberculosis (Mtb) to avoid innate host defense. In contrast, attenuated Mtb causes apoptosis, which limits bacterial replication and promotes T cell cross-priming by antigen-presenting cells. Here we show that Mtb infection causes plasma membrane microdisruptions. Resealing of these lesions, a process crucial for preventing necrosis and promoting apoptosis, required translocation of lysosomal and Golgi apparatus-derived vesicles to the plasma membrane. Plasma membrane repair depended on prostaglandin E(2) (PGE(2)), which regulates synaptotagmin 7 (Syt-7), the calcium sensor involved in the lysosome-mediated repair mechanism. By inducing production of lipoxin A(4) (LXA(4)), which blocks PGE(2) biosynthesis, virulent Mtb prevented membrane repair and induced necrosis. Thus, virulent Mtb impairs macrophage plasma membrane repair to evade host defenses.
诱导巨噬细胞坏死是毒力结核分枝杆菌(Mtb)用于逃避宿主固有防御的一种策略。相比之下,减毒Mtb会引发细胞凋亡,这会限制细菌复制并促进抗原呈递细胞对T细胞的交叉致敏。我们在此表明,Mtb感染会导致质膜微破裂。这些损伤的重新封闭是预防坏死和促进细胞凋亡的关键过程,需要溶酶体和高尔基体衍生的囊泡转运至质膜。质膜修复依赖于前列腺素E2(PGE2),它调节突触结合蛋白7(Syt-7),这是参与溶酶体介导的修复机制的钙传感器。通过诱导脂氧素A4(LXA4)的产生,其可阻断PGE2的生物合成,毒力Mtb可阻止膜修复并诱导坏死。因此,毒力Mtb会损害巨噬细胞质膜修复以逃避宿主防御。
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