首页> 外文期刊>Microcirculation: The official journal of the Microcirculatory Society >Regulation of blood-brain barrier permeability by transient receptor potential type C and type v calcium-permeable channels.
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Regulation of blood-brain barrier permeability by transient receptor potential type C and type v calcium-permeable channels.

机译:通过瞬时受体电位C型和V型钙渗透通道调节血脑屏障通透性。

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OBJECTIVE: To identify plasma membrane ion channels mediating calcium influx at the blood-brain barrier in response to disrupting stimuli. METHODS: We examined the expression and function of candidate transient receptor potential channels using reverse transcriptase polymerase chain recation, Fura-2 calcium imaging, and permeability assays. RESULTS: Immortalized mouse brain microvessel endothelial cells expressed multiple transient receptor potential isoforms: transient receptor potential C1, C2, C4, and C7, M2, M3, M4, and M7, and V2 and V4. Similar profiles were observed in freshly isolated cerebral microvessels and primary cultured rat brain endothelial cells. Thrombin-stimulated calcium influx in brain endothelial cells was blocked by transient receptor potential C inhibitors. Transient receptor potential V activating stimuli also increased intracellular calcium. This increase was inhibited by a transient receptor potential V blocker or by removal of extracellular calcium. Barrier integrity was compromised by thrombin, hypo-osmolar stress, and PMA treatment. The increase in barrier permeability induced by transient receptor potential V activators was blocked by transient receptor potential V inhibition, while thrombin effects were inhibited by transient receptor potential C inhibitors. CONCLUSIONS: These results demonstrate that transient receptor potential C and transient receptor potential V channels mediate calcium influx at the blood-brain barrier, and as a consequence, may modulate barrier integrity.
机译:目的:确定介导钙离子流入血脑屏障以应对破坏性刺激的质膜离子通道。方法:我们使用逆转录酶聚合酶链反应,Fura-2钙成像和通透性检测方法检查了候选瞬时受体潜在通道的表达和功能。结果:永生化的小鼠脑微血管内皮细胞表达多种瞬时受体电位亚型:瞬时受体电位C1,C2,C4和C7,M2,M3,M4和M7,以及V2和V4。在新鲜分离的脑微血管和原代培养的大鼠脑内皮细胞中观察到相似的轮廓。凝血酶刺激的脑内皮细胞钙流入被瞬时受体电位C抑制剂阻断。瞬态受体电位V激活刺激也增加了细胞内钙。这种增加被瞬时受体电位V受体阻滞剂或细胞外钙的去除所抑制。凝血酶,低渗压力和PMA处理会损害屏障的完整性。瞬时受体电势V激活剂诱导的屏障通透性增加被瞬时受体电势V抑制所阻止,而凝血酶作用被瞬时受体电势C抑制剂所抑制。结论:这些结果表明瞬时受体电位C和瞬时受体电位V通道介导血脑屏障的钙内流,因此可能调节屏障的完整性。

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