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Kinin receptors in cultured rat microglia.

机译:培养的大鼠小胶质细胞中的激肽受体。

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Kinins are produced and act at the site of injury and inflammation in various tissues. They are likely to initiate a particular cascade of inflammatory events, which evokes physiological and pathophysiological responses including an increase in blood flow and plasma leakage. In the central nervous system (CNS), kinins are potent stimulators of the production and release of pro-inflammatory mediators represented by prostanoids and cytotoxins. They are known to induce neural tissue damage. Many of the cytotoxins such as cytokines and free radicals and prostanoids are released from glial cells. Among glial cells, astrocytes and oligodendrocytes are known to possess bradykinin (BK) B(2) receptors that phosphoinositide (PI) turnover and raise intracellular Ca(2+) concentration. The presence of bradykinin receptors in microglia has been of great significance. We recently showed that rat primary microglia express kinin receptors. In resting microglia, B(2) receptors but not B(1) receptors are expressed. When the microglia are activated by bradykinin, B(1) receptors are up-regulated, while B(2) receptors are down-regulated. As observed in other glial cells, electrophysiological measurements suggest that B(2) receptors in phosphoinositide turnover and intracellular Ca(2+) concentration in microglia. Release of cytotoxins is likely consequent upon the activation of BK receptors. Our study provides the first evidence that microglia express functional kinin receptors and suggests that microglia play an important role in CNS inflammatory responses.
机译:激肽产生并作用于各种组织的损伤和炎症部位。它们很可能引发特定的炎症事件级联反应,从而引起生理和病理生理反应,包括血流增加和血浆渗漏。在中枢神经系统(CNS)中,激肽是产生和释放以前列腺素和细胞毒素为代表的促炎性介质的有效刺激剂。已知它们会引起神经组织损伤。神经胶质细胞释放出许多细胞毒素,例如细胞因子,自由基和类前列腺素。在胶质细胞中,星形胶质细胞和少突胶质细胞已知具有缓激肽(BK)B(2)受体,其磷酸肌醇(PI)转换并提高细胞内Ca(2+)的浓度。缓激肽受体在小胶质细胞中的存在具有重要意义。我们最近表明,大鼠原发性小胶质细胞表达激肽受体。在静息的小胶质细胞中,表达B(2)受体,但不表达B(1)受体。当小胶质细胞被缓激肽激活时,B(1)受体被上调,而B(2)受体被下调。正如在其他神经胶质细胞中观察到的那样,电生理测量表明,磷酸肌醇中的B(2)受体和小胶质细胞中的细胞内Ca(2+)浓度。 BK受体激活后可能会导致细胞毒素的释放。我们的研究提供了小胶质细胞表达功能性激肽受体的第一个证据,并表明小胶质细胞在中枢神经系统炎症反应中起重要作用。

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