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首页> 外文期刊>European Journal of Pharmacology: An International Journal >Early and sharp nitric oxide production and anoxic depolarization in the rat hippocampus during transient forebrain ischemia.
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Early and sharp nitric oxide production and anoxic depolarization in the rat hippocampus during transient forebrain ischemia.

机译:在短暂性前脑缺血期间,大鼠海马中早期和急剧的一氧化氮生成和缺氧去极化。

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This study was designed to characterize nitric oxide (NO) production and anoxic depolarization in the rat hippocampus during transient forebrain ischemia using two NO synthase (NOS) inhibitors, L-N(5)-(1-iminoethyl)ornithine (L-NIO), a relatively selective endothelial NOS (eNOS) inhibitor, and 7-nitroindazole, a relatively selective neuronal NOS (nNOS) inhibitor, and an NO scavenger, [2-(4-carboxyphenyl)-4,4,5,5-tetramethylimidazoline-1-oxyl-3-oxide] (carboxy-PTIO). We measured the mean arterial blood pressure, hippocampal blood flow, NO concentration and direct current potential before, during and after transient forebrain ischemia, which was induced by 4-vessel occlusion for 10 min. Saline, L-NIO (20 mg/kg), 7-nitroindazole (25 mg/kg), L-NIO (20 mg/kg)+7-nitroindazole (25 mg/kg) or carboxy-PTIO (1 mg/kg) was administered intraperitoneally 20 min before the onset of ischemia. We observed early and sharp NO production in the hippocampus during ischemia in the saline group. This NO increase during ischemia was significantly reduced by L-NIO (20 mg/kg)+7-nitroindazole (25 mg/kg) or carboxy-PTIO (1 mg/kg), but not L-NIO (20 mg/kg) or 7-nitroindazole (25 mg/kg). On the other hand, NO production after ischemia was significantly reduced by 7-nitroindazole (25 mg/kg), L-NIO (20 mg/kg)+7-nitroindazole (25 mg/kg) or carboxy-PTIO (1 mg/kg), but not L-NIO (20 mg/kg). The peak latency of NO production during ischemia always preceded the onset latency of anoxic depolarization in both the saline group and the carboxy-PTIO group. In the carboxy-PTIO group, the onset latency of anoxic depolarization was significantly longer than that in the saline group. Moreover, carboxy-PTIO significantly reduced the anoxic depolarization amplitude, compared with that of the saline group. These results suggest that both NOS-dependent and-independent NO formation contributes to early and sharp NO production during ischemia, and that this NO increase is, at least in part, related to the triggering of anoxic depolarization.
机译:这项研究旨在使用两种NO合酶(NOS)抑制剂LN(5)-(1-亚氨基乙基)鸟氨酸(L-NIO)来表征短暂性前脑缺血期间大鼠海马中一氧化氮(NO)的产生和缺氧去极化相对选择性的内皮NOS(eNOS)抑制剂和7-硝基吲唑,相对选择性的神经元NOS(nNOS)抑制剂和NO清除剂,[2-(4-羧基苯基)-4,4,5,5-四甲基咪唑啉-1-氧-3-氧化物](羧基-PTIO)。我们测量了短暂性前脑缺血之前,之中和之后的平均动脉血压,海马血流量,NO浓度和直流电势,这是由4血管闭塞10分钟引起的。盐水,L-NIO(20 mg / kg),7-硝基吲唑(25 mg / kg),L-NIO(20 mg / kg)+ 7-硝基吲唑(25 mg / kg)或羧基-PTIO(1 mg / kg在局部缺血开始前20分钟腹膜内给药。我们观察到盐水组在缺血期间海马中早期且急剧产生了一氧化氮。 L-NIO(20 mg / kg)+ 7-硝基吲唑(25 mg / kg)或羧基-PTIO(1 mg / kg)显着降低了缺血期间的NO升高,但L-NIO(20 mg / kg)没有明显降低或7-硝基吲唑(25 mg / kg)。另一方面,缺血后的NO生成量显着降低了7-硝基吲唑(25 mg / kg),L-NIO(20 mg / kg)+ 7-硝基吲唑(25 mg / kg)或羧基-PTIO(1 mg / kg公斤),但不含L-NIO(20毫克/公斤)。在盐水组和羧基-PTIO组中,缺血期间NO产生的峰值潜伏期总是先于缺氧去极化的发作潜伏期。在羧基-PTIO组,缺氧去极化的起始潜伏期明显长于生理盐水组。而且,与盐水组相比,羧基-PTIO显着降低了缺氧去极化幅度。这些结果表明,NOS依赖性和非依赖性NO的形成均有助于缺血期间早期和急剧的NO产生,并且这种NO增加至少部分地与引发缺氧去极化有关。

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