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P2X7 受体的新作用:在缺乏血清和细胞外 ATP 的情况下,作为细菌和凋亡细胞的清道夫受体。

A new role for the P2X7 receptor: a scavenger receptor for bacteria and apoptotic cells in the absence of serum and extracellular ATP.

机构信息

Florey Neuroscience Institutes, University of Melbourne, Parkville, VIC, 3010, Australia.

出版信息

Purinergic Signal. 2012 Sep;8(3):579-86. doi: 10.1007/s11302-012-9308-5. Epub 2012 Apr 4.

Abstract

The P2X7 receptor is widely recognized to mediate the proinflammatory effects of extracellular ATP. However this receptor in the absence of ATP may have a function unrelated to inflammation. Our data show that P2X7 expressed on the surface of monocyte/macrophages or on epithelial HEK-293 cells greatly augments the engulfment of latex beads and live and heat-killed bacteria by effector phagocyte in the absence of ATP and serum. The expression of P2X7 on the effector also confers the ability to phagocytose apoptotic target cells and an accumulation of P2X7 can be seen at the attachment point to the target. Activation of the P2X7 receptor by ATP causes a slow dissociation (over 10-15 min) of nonmuscle myosin from the P2X7 membrane complex and abolishes further P2X7-mediated phagocytosis of these targets. The recent crystal structure of the homologous zebrafish P2X4 receptor shows an exposed "nose" of the ectodomain (residues 115-162) which contains three of the five disulfide bonds conserved in all P2X receptors. Three short biotin-labeled peptides mimicking sequence of this exposed region bound to apoptotic target cells but not to either viable cells or to other target particles. All three peptides contained one or two cysteine residues and their replacement by alanine abolished peptide binding. These data implicate thiol-disulfide exchange reactions in the initial tethering of apoptotic cells to macrophage and establish P2X7 as one of the scavenger receptors involved in the recognition and removal of apoptotic cells in the absence of extracellular ATP and serum.

摘要

P2X7 受体被广泛认为介导细胞外 ATP 的促炎作用。然而,这种受体在没有 ATP 的情况下可能具有与炎症无关的功能。我们的数据表明,单核细胞/巨噬细胞表面或上皮 HEK-293 细胞表面表达的 P2X7 在没有 ATP 和血清的情况下大大增强了效应吞噬细胞对乳胶珠和活菌及热死菌的吞噬作用。效应物上 P2X7 的表达赋予了吞噬凋亡靶细胞的能力,并且可以在与靶细胞的附着点处看到 P2X7 的积累。ATP 激活 P2X7 受体导致非肌肉肌球蛋白从 P2X7 膜复合物缓慢解离(超过 10-15 分钟),并消除了对这些靶标的进一步 P2X7 介导的吞噬作用。最近同源斑马鱼 P2X4 受体的晶体结构显示出暴露的“鼻子”的外域(残基 115-162),其中包含所有 P2X 受体中保守的五个二硫键中的三个。三个短的生物素标记肽模拟该暴露区域的序列与凋亡靶细胞结合,但与活细胞或其他靶颗粒不结合。这三个肽都含有一个或两个半胱氨酸残基,其被丙氨酸取代会使肽结合丧失。这些数据表明,巯基-二硫键交换反应参与了凋亡细胞与巨噬细胞的初始连接,并确立了 P2X7 作为参与识别和清除无细胞外 ATP 和血清的凋亡细胞的吞噬受体之一。

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