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首页> 外文期刊>Brain research >Spinal taurine levels are increased 7 and 30 days following methylprednisolone treatment of spinal cord injury in rats.
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Spinal taurine levels are increased 7 and 30 days following methylprednisolone treatment of spinal cord injury in rats.

机译:甲基泼尼松龙治疗大鼠脊髓损伤后7和30天,脊髓牛磺酸水平升高。

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摘要

The amino acid taurine serves many functions in the nervous system serving as inhibitory neurotransmittereuromodulator, neurotrophin, antioxidant, and osmolyte. Taurine levels are increased following brain injury and glucocorticoid administration. Thus, the purpose of this study was to examine spinal taurine concentrations following spinal cord injury (SCI) and methylprednisolone (MP) treatment of SCI. A total of 44 adult male Sprague-Dawley rats were divided into control and lesion groups. Control rats received a T6 vertebral laminectomy while lesioned rats received a laminectomy followed by complete spinal transection. Half of the animals in each group received MP intravenously following sham-operation or SCI. Rats survived for 7 or 30 days and concentrations of taurine in spinal gray and white matter, in spinal segments both near and distant from the injury epicenter, were resolved by HPLC analysis. Taurine levels were increased 7 and 30 days following transection in spinal segments immediately adjacent to the lesion and were further elevated by MP treatment. No increases were seen in far rostral/caudal segments, and MP treatment alone had no effect on spinal taurine levels. These findings demonstrate that spinal injury results in increased taurine concentrations in spinal segments undergoing the greatest degree of cellular reactivity and tissue reorganization and that MP therapy potentiates these increases. These findings are significant in that they further characterize the effects of acute MP therapy in spinal tissue. Since taurine is thought to be involved in neuroprotection and/or regeneration following injury, the potentiation of taurine levels by MP treatment may relate to its therapeutic properties.
机译:氨基酸牛磺酸在神经系统中起着许多功能,可作为抑制性神经递质/神经调节剂,神经营养蛋白,抗氧化剂和渗透压物质。脑损伤和糖皮质激素给药后牛磺酸水平升高。因此,本研究的目的是检查脊髓损伤(SCI)和甲基强的松龙(MP)治疗脊髓损伤后的牛磺酸浓度。将总共​​44只成年雄性Sprague-Dawley大鼠分成对照组和病变组。对照大鼠接受了T6椎板椎板切除术,而病变大鼠接受了椎板切除术,随后进行了完整的脊椎横切术。在假手术或SCI后,每组一半的动物静脉注射MP。大鼠存活了7或30天,并且通过HPLC分析解决了在距损伤震中点近和远的脊髓节段中脊髓灰质和白质中牛磺酸的浓度。横断后第7天和第30天,紧邻病变的脊柱节段中的牛磺酸水平升高,而MP处理进一步提高了牛磺酸水平。在远鼻端/尾端节段未见增加,仅MP治疗对脊髓牛磺酸水平没有影响。这些发现表明,脊柱损伤导致经历最大程度的细胞反应性和组织重组的脊柱节段中牛磺酸浓度增加,而MP疗法可增强这些增加。这些发现是有意义的,因为它们进一步表征了急性MP疗法在脊柱组织中的作用。由于牛磺酸被认为与损伤后的神经保护和/或再生有关,因此通过MP处理增强牛磺酸水平可能与其治疗特性有关。

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