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UDP acting at P2Y_6 receptors is a mediator of microglial phagocytosis

机译:UDP作用于P2Y_6受体是小胶质细胞吞噬作用的介质

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Microglia, brain immune cells, engage in the clearance of dead cells or dangerous debris, which is crucial to the maintenance of brain functions. When a neighbouring cell is injured, microglia move rapidly towards it or extend a process to engulf the injured cell. Because cells release or leak ATP when they are stimulated or injured, extracellular nucleotides are thought to be involved in these events. In fact, ATP triggers a dynamic change in the motility of microglia in vitro and in vivo, a previously unrecognized mechanism underlying microglial chemotaxis; in contrast, microglial phagocytosis has received only limited attention. Here we show that microglia express the metabotropic P2Y_6 receptor whose activation by endogenous agonist UDP triggers microglial phagocytosis. UDP facilitated the uptake of microspheres in a P2Y_6-receptor-dependent manner, which was mimicked by the leakage of endogenous UDP when hippocampal neurons were damaged by kainic acid in vivo and in vitro. In addition, systemic administration of kainic acid in rats resulted in neuronal cell death in the hippocampal CA1 and CA3 regions, where increases in messenger RNA encoding P2Y_6 receptors that colocalized with activated microglia were observed. Thus, the P2Y_6 receptor is upregulated when neurons are damaged, and could function as a sensor for phagocytosis by sensing diffusible UDP signals, which is a previously unknown pathophysiological function of P2 receptors in microglia.
机译:小胶质细胞是大脑的免疫细胞,可清除死细胞或危险碎片,这对维持大脑功能至关重要。当相邻细胞受伤时,小胶质细胞会迅速向其移动或扩展吞噬受损细胞的过程。由于细胞在受到刺激或受伤时会释放或泄漏ATP,因此认为细胞外核苷酸与这些事件有关。实际上,ATP会在体外和体内触发小胶质细胞运动的动态变化,这是小胶质细胞趋化性之前无法识别的机制。相反,小胶质细胞吞噬作用仅受到了有限的关注。在这里,我们显示小胶质细胞表达代谢型P2Y_6受体,其通过内源性激动剂UDP的激活触发小胶质细胞吞噬作用。 UDP以P2Y_6受体依赖性方式促进微球的摄取,当海马酸在体内和体外破坏海马神经元时,内源UDP的泄漏模拟了UDP。此外,在大鼠中全身施用海藻酸会导致海马CA1和CA3区神经元细胞死亡,其中观察到与活化的小胶质细胞共定位的编码P2Y_6受体的信使RNA的增加。因此,当神经元受损时,P2Y_6受体被上调,并且可以通过感测可扩散的UDP信号充当吞噬作用的传感器,这是小胶质细胞中P2受体先前未知的病理生理功能。

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