镁治疗对脑缺血疾病的神经保护作用。

Thomas Westermaier, Christian Stetter, Ekkehard Kunze, Nadine Willner, Furat Raslan, Giles H Vince, Ralf-Ingo Ernestus
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摘要

本文回顾了在各种脑缺血情况下使用镁作为神经保护剂的实验和临床数据。虽然镁在全局性和局灶性脑缺血的动物模型中显示出神经保护特性,但在大型人类中风试验中却无法再现这种效果。这些相互矛盾的结果可能与治疗时机有关。在实验研究中,治疗可以在缺血前或缺血后早期开始,但在人类中风中,治疗不可避免地会出现延迟。在几项随机对照试验中,对有早产风险的妇女服用镁进行了研究,发现镁可降低早产儿出现神经功能缺损的风险。一些对照临床试验对围产期窒息后的婴儿产后服用镁进行了研究。研究结果很有希望,但迄今为止,这些试验的效果还不够理想。在动脉瘤性蛛网膜下腔出血(SAH)中,动脉瘤破裂数天后,随着延迟性脑血管痉挛的发生,会出现脑缺血。与即将早产的围产期窒息相似,可以在缺血之前开始治疗。临床试验的结果相互矛盾。几项临床试验并未显示镁与尼莫地平(许多中心对 SAH 患者常规使用的另一种钙拮抗剂)的叠加效应。其他试验则发现镁治疗后有保护作用。因此,在治疗动脉瘤性 SAH 后的继发性脑缺血方面,镁仍是一种很有前景的物质。本文讨论了镁治疗的未来前景。
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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Magnesium treatment for neuroprotection in ischemic diseases of the brain.

This article reviews experimental and clinical data on the use of magnesium as a neuroprotective agent in various conditions of cerebral ischemia. Whereas magnesium has shown neuroprotective properties in animal models of global and focal cerebral ischemia, this effect could not be reproduced in a large human stroke trial. These conflicting results may be explained by the timing of treatment. While treatment can be started before or early after ischemia in experimental studies, there is an inevitable delay of treatment in human stroke. Magnesium administration to women at risk for preterm birth has been investigated in several randomized controlled trials and was found to reduce the risk of neurological deficits for the premature infant. Postnatal administration of magnesium to babies after perinatal asphyxia has been studied in a number of controlled clinical trials. The results are promising but the trials have, so far, been underpowered. In aneurysmal subarachnoid hemorrhage (SAH), cerebral ischemia arises with the onset of delayed cerebral vasospasm several days after aneurysm rupture. Similar to perinatal asphyxia in impending preterm delivery, treatment can be started prior to ischemia. The results of clinical trials are conflicting. Several clinical trials did not show an additive effect of magnesium with nimodipine, another calcium antagonist which is routinely administered to SAH patients in many centers. Other trials found a protective effect after magnesium therapy. Thus, it may still be a promising substance in the treatment of secondary cerebral ischemia after aneurysmal SAH. Future prospects of magnesium therapy are discussed.

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