Janáky R, Shaw C A, Oja S S, Saransaari P
Brain Research Center, University of Tampere Medical School, Tampere, Finland.
Amino Acids. 2008 Jan;34(1):75-80. doi: 10.1007/s00726-007-0587-z. Epub 2007 Aug 15.
Glutathione (reduced form GSH and oxidized form GSSG) constitutes an important defense against oxidative stress in the brain, and taurine is an inhibitory neuromodulator particularly in the developing brain. The effects of GSH and GSSG and glycylglycine, gamma-glutamylcysteine, cysteinylglycine, glycine and cysteine on the release of [(3)H]taurine evoked by K+-depolarization or the ionotropic glutamate receptor agonists glutamate, kainate, 2-amino-3-hydroxy-5-methyl-4-isoxazolepropionate (AMPA) and N-methyl-D-aspartate (NMDA) were now studied in slices from the hippocampi from 7-day-old mouse pups in a perfusion system. All stimulatory agents (50 mM K(+), 1 mM glutamate, 0.1 mM kainate, 0.1 mM AMPA and 0.1 mM NMDA) evoked taurine release in a receptor-mediated manner. Both GSH and GSSG significantly inhibited the release evoked by 50 mM K+. The release induced by AMPA and glutamate was also inhibited, while the kainate-evoked release was significantly activated by both GSH and GSSG. The NMDA-evoked release proved the most sensitive to modulation: L-Cysteine and glycine enhanced the release in a concentration-dependent manner, whereas GSH and GSSG were inhibitory at low (0.1 mM) but not at higher (1 or 10 mM) concentrations. The release evoked by 0.1 mM AMPA was inhibited by gamma-glutamylcysteine and cysteinylglycine, whereas glycylglycine had no effect. The 0.1 mM NMDA-evoked release was inhibited by glycylglycine and gamma-glutamylcysteine. In turn, cysteinylglycine inhibited the NMDA-evoked release at 0.1 mM, but was inactive at 1 mM. Glutathione exhibited both enhancing and attenuating effects on taurine release, depending on the glutathione concentration and on the agonist used. Both glutathione and taurine act as endogenous neuroprotective effectors during early postnatal life.
谷胱甘肽(还原型GSH和氧化型GSSG)是大脑抵御氧化应激的重要防线,而牛磺酸是一种抑制性神经调节剂,尤其在发育中的大脑中。本研究在灌注系统中,对7日龄小鼠幼崽海马体切片中,GSH、GSSG、甘氨酰甘氨酸、γ-谷氨酰半胱氨酸、半胱氨酰甘氨酸、甘氨酸和半胱氨酸对K⁺去极化或离子型谷氨酸受体激动剂谷氨酸、海人酸、2-氨基-3-羟基-5-甲基-4-异恶唑丙酸(AMPA)和N-甲基-D-天冬氨酸(NMDA)诱发的[³H]牛磺酸释放的影响进行了研究。所有刺激剂(50 mM K⁺、1 mM谷氨酸、0.1 mM海人酸、0.1 mM AMPA和0.1 mM NMDA)均以受体介导的方式诱发牛磺酸释放。GSH和GSSG均显著抑制50 mM K⁺诱发的释放。AMPA和谷氨酸诱发的释放也受到抑制,而海人酸诱发的释放则被GSH和GSSG显著激活。NMDA诱发的释放对调节最为敏感:L-半胱氨酸和甘氨酸以浓度依赖的方式增强释放,而GSH和GSSG在低浓度(0.1 mM)时具有抑制作用,但在较高浓度(1或10 mM)时则无此作用。0.1 mM AMPA诱发的释放被γ-谷氨酰半胱氨酸和半胱氨酰甘氨酸抑制,而甘氨酰甘氨酸则无作用。0.1 mM NMDA诱发的释放被甘氨酰甘氨酸和γ-谷氨酰半胱氨酸抑制。反过来,半胱氨酰甘氨酸在0.1 mM时抑制NMDA诱发的释放,但在1 mM时无活性。谷胱甘肽对牛磺酸释放具有增强和减弱两种作用,这取决于谷胱甘肽的浓度和所使用的激动剂。在出生后的早期生活中,谷胱甘肽和牛磺酸均作为内源性神经保护效应物发挥作用。