Inflammatory Cytokines Facilitate the Sensitivity of P2X7 Receptors Toward Extracellular ATP at Neural Progenitor Cells of the Rodent Hippocampal Subgranular Zone

Juan Liu, M. T. Khan, Yong Tang, H. Franke, P. Illés
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Abstract

Organotypic hippocampal slice cultures were used to model the effects of neuroinflammatory conditions following an epileptic state on functional P2X7 receptors (Rs) of subgranular zone (SGZ) neural progenitor cells (NPCs). The compound, 4-aminopyridine (4-AP), is known to cause pathological firing of neurons, consequently facilitating the release of various transmitter substances including ATP. Lipopolysaccharide (LPS) and interleukin-1β (IL-1β) both potentiated the dibenzoyl-ATP (Bz-ATP)-induced current amplitudes in NPCs, although via different mechanisms. Whereas LPS acted via promoting ATP release, IL-1β acted via its own receptor to directly influence P2X7Rs. Thus, the effect of LPS was inhibited by the ecto-ATPase inhibitor, apyrase, but not by the IL-1β antagonist, interleukin-1RA (IL-1RA); by contrast, the effect of IL-1β was inhibited by IL-1RA, but not by apyrase. Eventually, incubation with 4-AP upregulated the number of nestin/glial fibrillary acidic protein/P2X7R immunoreactive cells and their appropriate staining intensity, suggesting increased synthesis of P2X7Rs at NPCs. In conclusion, inflammatory cytokines accumulating after epilepsy-like neuronal firing may facilitate the effect of endogenous ATP at P2X7Rs of NPCs, thereby probably promoting necrosis/apoptosis and subsequent cell death.
炎症细胞因子促进P2X7受体对啮齿动物海马亚颗粒区神经祖细胞细胞外ATP的敏感性
使用器官型海马切片培养物来模拟癫痫状态后神经炎症条件对颗粒下区(SGZ)神经祖细胞(NPC)功能性P2X7受体(Rs)的影响。已知化合物4-氨基吡啶(4-AP)会引起神经元的病理性放电,从而促进包括ATP在内的各种递质的释放。脂多糖(LPS)和白细胞介素-1β(IL-1β)均通过不同的机制增强了二苯甲酰ATP(Bz-ATP)诱导的NPC电流振幅。LPS通过促进ATP释放发挥作用,IL-1β通过自身受体直接影响P2X7Rs。因此,LPS的作用被胞外ATP酶抑制剂apyrase抑制,但不被IL-1β拮抗剂白细胞介素-1RA(IL-1RA)抑制;相反,IL-1RA对IL-1β的作用有抑制作用,而apyrase则没有。最终,与4-AP孵育上调了巢蛋白/神经胶质原纤维酸性蛋白/P2X7R免疫反应细胞的数量及其适当的染色强度,表明在NPC处P2X7R的合成增加。总之,癫痫样神经元放电后积累的炎性细胞因子可能促进内源性ATP对NPC P2X7Rs的作用,从而可能促进坏死/凋亡和随后的细胞死亡。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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