特定的 P2X₇ 受体拮抗剂的神经保护作用源自其抑制神经胶质细胞中 NLRP3 炎性小体组装的能力。
The neuroprotective effect of a specific P2X₇ receptor antagonist derives from its ability to inhibit assembly of the NLRP3 inflammasome in glial cells.
机构信息
Trinity College Institute for Neuroscience, Physiology Department, Trinity College, Dublin, Ireland.
出版信息
Brain Pathol. 2012 May;22(3):295-306. doi: 10.1111/j.1750-3639.2011.00531.x. Epub 2011 Oct 27.
Abstract
Release of interleukin (IL)-1β from immunocompetent cells requires formation of the NACHT, LLR and PYD domains-containing protein 3 (NLRP3) inflammasome and caspase 1 activation. Adenosine 5'-triphosphate (ATP), acting on the P2X(7) receptor, is one factor that stimulates inflammasome assembly. We show that a novel specific P2X(7) receptor antagonist, GSK1370319A, inhibits ATP-induced increase in IL-1β release and caspase 1 activation in lipopolysaccharide (LPS)-primed mixed glia by blocking assembly of the inflammasome in a pannexin 1-dependent manner. GSK1370319A also inhibits ATP-induced subregion-specific neuronal loss in hippocampal organotypic slice cultures, which is dependent on its ability to prevent inflammasome assembly in glia. Significantly, GSK1370319A attenuates age-related deficits in long-term potentiation (LTP) and inhibits the accompanying age-related caspase 1 activity. We conclude that inhibiting P2X(7) receptor-activated NLRP3 inflammasome formation and the consequent IL-1β release from glia preserve neuronal viability and synaptic activity.
摘要
免疫活性细胞中白细胞介素 (IL)-1β的释放需要 NACHT、LLR 和 PYD 结构域包含蛋白 3 (NLRP3) 炎症小体的形成和半胱天冬酶 1 的激活。三磷酸腺苷 (ATP) 通过作用于 P2X(7) 受体,是刺激炎症小体组装的一个因素。我们发现,一种新型的特异性 P2X(7) 受体拮抗剂 GSK1370319A 通过以连接蛋白 1 依赖性方式阻断炎症小体的组装,抑制脂多糖 (LPS) 预激活的混合神经胶质细胞中 ATP 诱导的 IL-1β释放和半胱天冬酶 1 的激活。GSK1370319A 还抑制海马器官型切片培养物中 ATP 诱导的亚区特异性神经元丢失,这依赖于其在神经胶质细胞中阻止炎症小体组装的能力。重要的是,GSK1370319A 减轻了与年龄相关的长时程增强 (LTP) 缺陷,并抑制了伴随的与年龄相关的半胱天冬酶 1 活性。我们得出结论,抑制 P2X(7) 受体激活的 NLRP3 炎症小体形成以及随后从神经胶质细胞中释放白细胞介素-1β可维持神经元活力和突触活性。
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