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首页> 外文期刊>Neuropharmacology >Pharmacological assessment of the role of the glycine transporter GlyT-1 in mediating high-affinity glycine uptake by rat cerebral cortex and cerebellum synaptosomes.
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Pharmacological assessment of the role of the glycine transporter GlyT-1 in mediating high-affinity glycine uptake by rat cerebral cortex and cerebellum synaptosomes.

机译:甘氨酸转运蛋白GlyT-1在介导大鼠大脑皮层和小脑突触体高亲和力甘氨酸摄取中的作用的药理学评估。

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Two distinct types of glycine transporter, GlyT-1 and GlyT-2, have been characterised. GlyT-1 and GlyT-2 are known to be differentially expressed amongst CNS areas, but direct functional evidence for their relative contributions to high-affinity glycine uptake by brain tissues is lacking. In the present study, we have used the selective GlyT-1 inhibitor N[3-(4"-fluorophenyl)-3-(4"-phenylphenoxy)propyl]sarcosine (NFPS) to investigate the role of GlyT-1 in mediating glycine uptake. HEK293 cells expressing human GlyT-1c or GlyT-2 showed high levels of Na(+)-dependent glycine uptake, with K(m) values of 117+/-13 and 200+/-22 microM, respectively. NFPS potently inhibited uptake in GlyT-1c cells (IC(50) value 0.22+/-0.03 microM), being around 500-fold more potent than glycine or sarcosine, but had no effect on uptake in GlyT-2 cells (IC(50) >10 microM). Efflux of pre-loaded [3H]-glycine from GlyT-1c cells was increased by glycine or sarcosine, whereas NFPS had no effect on its own but blocked the effects of glycine or sarcosine. These results confirm that NFPS is a potent, selective and non-transportable GlyT-1 inhibitor. Rat cortex and cerebellum synaptosomes also showed a high-affinity Na(+)-dependent component of glycine uptake, with affinities similar to those observed for uptake in GlyT-1c or GlyT-2 cells. In cortex synaptosomes, NFPS and sarcosine produced the same maximal inhibition of uptake as glycine itself. However, in cerebellum synaptosomes, the maximal inhibition produced by NFPS and sarcosine was only half that produced by glycine. In both tissues NFPS was around 1000-fold more potent than glycine or sarcosine. Overall, our findings indicate that high-affinity glycine uptake in cerebral cortex occurs predominantly via GlyT-1. However, in cerebellum, only a part of the high-affinity uptake is mediated by GlyT-1, with the remaining NFPS-insensitive component most likely mediated by GlyT-2.
机译:已经表征了两种不同类型的甘氨酸转运蛋白,GlyT-1和GlyT-2。已知GlyT-1和GlyT-2在中枢神经系统区域中差异表达,但缺乏直接的功能性证据证明它们对脑组织对高亲和力甘氨酸的吸收有相对贡献。在本研究中,我们已经使用了选择性GlyT-1抑制剂N [3-(4“-氟苯基)-3-(4”-苯基苯氧基)丙基]肌氨酸(NFPS)来研究GlyT-1在介导甘氨酸中的作用摄取。表达人GlyT-1c或GlyT-2的HEK293细胞显示高水平的Na(+)依赖性甘氨酸摄取,K(m)值分别为117 +/- 13和200 +/- 22 microM。 NFPS有效抑制GlyT-1c细胞的摄取(IC(50)值0.22 +/- 0.03 microM),效力比甘氨酸或肌氨酸强约500倍,但对GlyT-2细胞的摄取没有影响(IC(50 )> 10 microM)。甘氨酸或肌氨酸增加了来自GlyT-1c细胞的[3H]-甘氨酸的外排,而NFPS本身没有作用,但阻止了甘氨酸或肌氨酸的作用。这些结果证实了NFPS是一种有效的,选择性的和不可运输的GlyT-1抑制剂。大鼠皮层和小脑突触体也显示了甘氨酸摄取的高亲和力Na(+)依赖成分,其亲和力类似于在GlyT-1c或GlyT-2细胞中观察到的亲和力。在皮质突触小体中,NFPS和肌氨酸产生的吸收抑制作用与甘氨酸本身相同。但是,在小脑突触小体中,NFPS和肌氨酸产生的最大抑制作用仅是甘氨酸产生的抑制作用的一半。在两个组织中,NFPS的效力都比甘氨酸或肌氨酸强约1000倍。总体而言,我们的研究结果表明,大脑皮层中高亲和力甘氨酸的摄取主要通过GlyT-1发生。但是,在小脑中,高亲和力摄取中只有一部分是由GlyT-1介导的,而其余的NFPS不敏感成分很可能是由GlyT-2介导的。

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