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首页> 外文期刊>Stroke: A Journal of Cerebral Circulation >Factors influencing the frequency of fluorescence transients as markers of peri-infarct depolarizations in focal cerebral ischemia.
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Factors influencing the frequency of fluorescence transients as markers of peri-infarct depolarizations in focal cerebral ischemia.

机译:影响局灶性脑缺血中梗死周围去极化的荧光瞬变频率的因素。

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摘要

BACKGROUND AND PURPOSE: Peri-infarct depolarizations (PIDs) that occur in ischemic boundary zones of the cerebral cortex of experimental animals have been shown to promote rather than simply to indicate the evolution of the lesion and are especially prominent in the rat. To study the influence of one factor, species, on PID incidence, we compared the frequency of PIDs in a primate species, the squirrel monkey, with that in the cat after middle cerebral artery occlusion. Plasma glucose was reviewed as a possible cause of interexperiment variability in the cat experiments. METHODS: In open-skull experiments under chloralose anesthesia, changes in cortical fluorescence believed to indicate NADH/NAD(+) redox state, as markers of PIDs, were recorded by serial imaging of the cortical surface in vivo for 4 hours after middle cerebral artery occlusion. RESULTS: Fluorescence transients occurred in squirrel monkeys at a frequency (mean+/-SD) of 0.7+/-0.8 hours(-1) (n=5), which was not significantly less than in that observed in cats (1.3+/-1.6 hours(-1), n=8). Data from the cat experiments indicated a relationship between number of transients (dependent) and plasma glucose, with a striking increase in PID frequency in association with values of mean postocclusion plasma glucose <4.1 mmol/L (Mann-Whitney U=15.0, P=0.034); this observation agrees well with other published findings. CONCLUSIONS: Transient changes in fluorescence strongly suggestive of peri-infarct depolarizations, either transient or terminal, occur and propagate in the ischemic cerebral cortex of a nonhuman primate. The results also suggest that the relationship of frequency of peri-infarct depolarizations with plasma glucose requires further examination, to confirm the finding and to determine a safe lower limit for a target range for control of plasma glucose if insulin is used in the management of patients with cerebral ischemia.
机译:背景与目的:实验动物的大脑皮质缺血边界区域发生的梗死周围去极化(PID)已被证明可以促进而不是简单地指示病变的发展,并且在大鼠中尤其明显。为了研究一个因素物种对PID发生率的影响,我们比较了灵长类动物,松鼠猴和大脑中动脉闭塞后猫中PID的发生频率。在猫实验中,血浆葡萄糖被认为是实验间差异的可能原因。方法:在氯醛糖麻醉下的开颅实验中,通过大脑中动脉后4小时的体内皮质表面连续成像,记录了皮质荧光变化(据信指示NADH / NAD(+)氧化还原状态,作为PID的标记)。闭塞。结果:松鼠猴的荧光瞬变发生频率为0.7 +/- 0.8小时(-1)(n = 5)(平均值±标准差),与猫的观察频率(1.3 +/- 1.6小时(-1),n = 8)。猫实验的数据表明,瞬态次数(依赖性)与血浆葡萄糖之间存在关系,PID频率显着增加,与平均闭塞后血浆葡萄糖值<4.1 mmol / L有关(Mann-Whitney U = 15.0,P = 0.034);这一观察结果与其他已发表的发现非常吻合。结论:荧光的瞬时变化强烈提示在非人灵长类动物的缺血性大脑皮层中发生并传播了梗死周围的去极化,无论是短暂的还是末端的。结果还表明,如果在患者的治疗中使用胰岛素,则需要进一步检查梗死周围去极化频率与血浆葡萄糖的关系,以确认该发现并确定血浆葡萄糖控制目标范围的安全下限。脑缺血。

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