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一种丝氨酸蛋白酶原作为脂多糖的模式识别受体发挥作用。

A serine protease zymogen functions as a pattern-recognition receptor for lipopolysaccharides.

作者信息

Ariki Shigeru, Koori Kumiko, Osaki Tsukasa, Motoyama Kiyohito, Inamori Kei-ichiro, Kawabata Shun-ichiro

机构信息

Department of Biology, Faculty of Sciences, Kyushu University, Fukuoka 812-8581, Japan.

出版信息

Proc Natl Acad Sci U S A. 2004 Jan 27;101(4):953-8. doi: 10.1073/pnas.0306904101. Epub 2004 Jan 13.

Abstract

Bacterial lipopolysaccharide (LPS)-induced exocytosis of granular hemocytes is a key component of the horseshoe crab's innate immunity to infectious microorganisms; stimulation by LPS induces the secretion of various defense molecules from the granular hemocytes. Using a previously uncharacterized assay for exocytosis, we clearly show that hemocytes respond only to LPS and not to other pathogen-associated molecular patterns, such as beta-1,3-glucans and peptidoglycans. Furthermore, we show that a granular protein called factor C, an LPS-recognizing serine protease zymogen that initiates the hemolymph coagulation cascade, also exists on the hemocyte surface as a biosensor for LPS. Our data demonstrate that the proteolytic activity of factor C is both necessary and sufficient to trigger exocytosis through a heterotrimeric GTP-binding protein-mediating signaling pathway. Exocytosis of hemocytes was not induced by thrombin, but it was induced by hexapeptides corresponding to the tethered ligands of protease-activated G protein-coupled receptors (PARs). This finding suggested the presence of a PAR-like receptor on the hemocyte surface. We conclude that the serine protease zymogen on the hemocyte surface functions as a pattern-recognition protein for LPS.

摘要

细菌脂多糖(LPS)诱导颗粒血细胞的胞吐作用是鲎对感染性微生物固有免疫的关键组成部分;LPS刺激可诱导颗粒血细胞分泌多种防御分子。通过一种以前未被描述的胞吐作用检测方法,我们清楚地表明血细胞仅对LPS有反应,而对其他病原体相关分子模式,如β-1,3-葡聚糖和肽聚糖无反应。此外,我们表明一种名为C因子的颗粒蛋白,一种启动血淋巴凝固级联反应的LPS识别丝氨酸蛋白酶原,也作为LPS的生物传感器存在于血细胞表面。我们的数据表明,C因子的蛋白水解活性对于通过异源三聚体GTP结合蛋白介导的信号通路触发胞吐作用既是必要的也是充分的。凝血酶不会诱导血细胞的胞吐作用,但对应于蛋白酶激活的G蛋白偶联受体(PARs)的拴系配体的六肽会诱导胞吐作用。这一发现表明血细胞表面存在一种类似PAR的受体。我们得出结论,血细胞表面的丝氨酸蛋白酶原作为LPS的模式识别蛋白发挥作用。

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