首页> 外文期刊>Journal of Neurochemistry: Offical Journal of the International Society for Neurochemistry >Nitric oxide production and perivascular tyrosine nitration following focal ischemia in neonatal rat.
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Nitric oxide production and perivascular tyrosine nitration following focal ischemia in neonatal rat.

机译:新生鼠局灶性缺血后一氧化氮的产生和血管周围酪氨酸的硝化

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摘要

Oxygen free radicals and nitric oxide (NO.) have been proposed to be involved in acute CNS injury produced by cerebral ischemia; however, controversy remains regarding how they cause injury. Because superoxide generation is triggered during reperfusion, the cytotoxic oxidant peroxynitrite could be formed, but it is not known if this occurs. Dot blot and immunohistochemistry studies were performed on the magnitude and time course of tyrosine nitration and inducible NO synthase (NOS2) in the postischemic rat pup brain. Neonatal ischemia was induced by permanent left middle cerebral artery occlusion in association with 1-h occlusion of the left common carotid artery in 7-day-old Wistar pups. Nitrotyrosine (NT) immunoreactivity was evident in the blood vessels close to the cortical infarct at 48-72 h of recovery, and T lymphocytes were involved with this production. NOS2 immunoreactivity was seen in neutrophils in the same vessels and in the parenchyma at 72 h of recirculation. Whereas NT staining decreased with time, NOS2-positive neutrophils could be still detected in arachnoid vessels at 14 days of recirculation. We conclude that perivascular reactions mediated by peroxynitrite are important in the cascade of events that lead to brain oxidative stress in neonatal ischemia. Moreover, NO-related species may serve as a signaling function instead of directly mediating toxicity.
机译:已经提出氧自由基和一氧化氮(NO。)与脑缺血引起的急性中枢神经系统损伤有关。然而,关于它们如何造成伤害的争议仍然存在。由于在再灌注过程中会触发超氧化物的产生,因此会形成细胞毒性氧化剂过氧亚硝酸盐,但尚不清楚是否会发生。对缺血后大鼠小脑中酪氨酸硝化和诱导型NO合酶(NOS2)的大小和时间进行了斑点印迹和免疫组化研究。在7天大的Wistar幼崽中,永久性左大脑中动脉闭塞与左颈总动脉1小时闭塞相结合可诱发新生儿缺血。在恢复48-72小时后,在靠近皮层梗死的血管中明显出现了硝基酪氨酸(NT)免疫反应,并且T淋巴细胞参与了该产生。在再循环的72小时内,在同一血管的中性粒细胞和实质中可见NOS2免疫反应性。尽管NT染色随时间下降,但在再循环的第14天,仍可在蛛网膜血管中检测到NOS2阳性中性粒细胞。我们得出结论,过氧亚硝酸盐介导的血管周围反应在导致新生儿缺血的脑部氧化应激的一系列事件中很重要。此外,NO相关物种可以充当信号功能,而不是直接介导毒性。

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