Department of Neurological Surgery, University of California at Davis, One Shields Avenue, Davis, CA 95616, USA.
Brain Res. 2013 Jun 17;1515:98-107. doi: 10.1016/j.brainres.2013.03.043. Epub 2013 Apr 3.
Immediately following traumatic brain injury (TBI) and TBI with hypoxia, there is a rapid and pathophysiological increase in extracellular glutamate, subsequent neuronal damage and ultimately diminished motor and cognitive function. N-acetyl-aspartyl glutamate (NAAG), a prevalent neuropeptide in the CNS, is co-released with glutamate, binds to the presynaptic group II metabotropic glutamate receptor subtype 3 (mGluR3) and suppresses glutamate release. However, the catalytic enzyme glutamate carboxypeptidase II (GCP II) rapidly hydrolyzes NAAG into NAA and glutamate. Inhibition of the GCP II enzyme with NAAG peptidase inhibitors reduces the concentration of glutamate both by increasing the duration of NAAG activity on mGluR3 and by reducing degradation into NAA and glutamate resulting in reduced cell death in models of TBI and TBI with hypoxia. In the following study, rats were administered the NAAG peptidase inhibitor PGI-02776 (10mg/kg) 30 min following TBI combined with a hypoxic second insult. Over the two weeks following injury, PGI-02776-treated rats had significantly improved motor function as measured by increased duration on the rota-rod and a trend toward improved performance on the beam walk. Furthermore, two weeks post-injury, PGI-02776-treated animals had a significant decrease in latency to find the target platform in the Morris water maze as compared to vehicle-treated animals. These findings demonstrate that the application of NAAG peptidase inhibitors can reduce the deleterious motor and cognitive effects of TBI combined with a second hypoxic insult in the weeks following injury.
在创伤性脑损伤(TBI)和伴有缺氧的 TBI 后,细胞外谷氨酸迅速增加,导致病理生理学变化,随后神经元受损,最终运动和认知功能下降。N-乙酰天冬氨酸谷氨酸(NAAG)是中枢神经系统中一种常见的神经肽,与谷氨酸共同释放,与突触前 2 型代谢型谷氨酸受体亚型 3(mGluR3)结合,抑制谷氨酸释放。然而,谷氨酸羧肽酶 II(GCP II)的催化酶迅速将 NAAG 水解为 NAA 和谷氨酸。用 NAAG 肽酶抑制剂抑制 GCP II 酶,通过增加 NAAG 在 mGluR3 上的活性持续时间以及减少降解为 NAA 和谷氨酸来降低谷氨酸浓度,从而减少 TBI 和伴有缺氧的 TBI 模型中的细胞死亡。在接下来的研究中,大鼠在 TBI 合并缺氧二次打击后 30 分钟给予 NAAG 肽酶抑制剂 PGI-02776(10mg/kg)。在损伤后两周内,PGI-02776 治疗的大鼠在旋转棒上的持续时间增加,在横梁行走上的表现有改善趋势,运动功能明显改善。此外,损伤后两周,PGI-02776 治疗的动物在 Morris 水迷宫中找到目标平台的潜伏期明显短于载体治疗的动物。这些发现表明,应用 NAAG 肽酶抑制剂可以减少损伤后数周内 TBI 合并二次缺氧打击引起的运动和认知损伤。