Progesterone protects against lipid peroxidation following traumatic brain injury in rats.

R L Roof, S W Hoffman, D G Stein
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引用次数: 306

Abstract

The gonadal hormone, progesterone, has been shown to have neuroprotective effects in injured nervous system, including the severity of postinjury cerebral edema. Progesterone's attenuation of edema is accompanied by a sparing of neurons from secondary neuronal death and with improvements in cognitive outcome. In addition, we recently reported that postinjury blood-brain barrier (BBB) leakage, as measured by albumin immunostaining, was significantly lower in progesterone treated than in nontreated rats, supporting a possible protective action of progesterone on the BBB. Because lipid membrane peroxidation is a major contributor to BBB breakdown, we hypothesized that progesterone limits this free radical-induced damage. An antioxidant action, neuroprotective in itself, would also account for progesterone's effects on the BBB, edema, and cell survival after traumatic brain injury. To test progesterone's possible antiperoxidation effect, we compared brain levels of 8-isoprostaglandin F2 alpha (8-isoPGF2 alpha), a marker of lipid peroxidation, 24, 48, and 72 h after cortical contusion in male rats treated with either progesterone or the oil vehicle. The brains of progesterone treated rats contained approximately one-third of the 8-isoPGF2 alpha found in oil-treated rats. These data suggest progesterone has antioxidant effects and support its potential as a treatment for brain injury.

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黄体酮对大鼠创伤性脑损伤后脂质过氧化的保护作用。
性激素黄体酮已被证明对受伤的神经系统有神经保护作用,包括严重的损伤后脑水肿。黄体酮对水肿的抑制伴随着继发性神经元死亡神经元的保留和认知结果的改善。此外,我们最近报道,通过白蛋白免疫染色测量,孕酮治疗的大鼠损伤后血脑屏障(BBB)渗漏明显低于未治疗的大鼠,支持孕酮对血脑屏障的可能保护作用。由于脂质膜过氧化是血脑屏障分解的主要原因,我们假设黄体酮限制了这种自由基诱导的损伤。抗氧化作用,本身的神经保护作用,也可以解释黄体酮对脑外伤后血脑屏障、水肿和细胞存活的影响。为了测试孕酮可能的抗氧化作用,我们比较了8-异前列腺素F2 α (8-isoPGF2 α)的脑水平,这是脂质过氧化的标志,在皮质挫伤后24、48和72小时,雄性大鼠分别接受孕酮或油处理。孕酮处理大鼠的大脑中含有的8-isoPGF2 α大约是油处理大鼠的三分之一。这些数据表明黄体酮具有抗氧化作用,并支持其治疗脑损伤的潜力。
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