首页> 外文期刊>Journal of Neurochemistry: Offical Journal of the International Society for Neurochemistry >Down-regulation of norepinephrine transporters on PC12 cells by transporter inhibitors.
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Down-regulation of norepinephrine transporters on PC12 cells by transporter inhibitors.

机译:转运蛋白抑制剂对PC12细胞上去甲肾上腺素转运蛋白的下调。

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摘要

To investigate the regulation of norepinephrine transporters (NETs) in vitro, we measured the binding of the NET-selective ligand [3H]nisoxetine in homogenates of PC12 cells after exposure of intact cells to the NET inhibitor desipramine (DMI). A 3-day exposure of PC12 cells to DMI robustly reduced the Bmax, but not the KD, of [3H]nisoxetine binding to NETs. Reduction of the binding of [3H]nisoxetine was dependent on both the concentration of DMI and the time of exposure to DMI. Reduction of [3H]nisoxetine binding to NETs produced by a 1-day exposure to DMI reverted to preexposure levels 48 h after cessation of DMI exposure. Similar down-regulation of NETs was found when PC12 cells were exposed to another NET-selective drug, nisoxetine, which is structurally unrelated to DMI. In contrast, exposure of cells to the serotonin transporter-selective drug citalopram, or the NET substrate norepinephrine, had no effects on the binding of [3H]nisoxetine to NETs. The down-regulation of NETs was paralleled by a DMI-induced reduction in the uptake of [3H]norepinephrine in intact PC12 cells. It can be inferred from these data that inhibitors of the NET can down-regulate NETs directly, and do so in the absence of changes in the synaptic concentration of norepinephrine.
机译:为了研究去甲肾上腺素转运蛋白(NETs)的体外调控,我们测量了NET选择性配体[3H] nisoxetine在完整细胞暴露于NET抑制剂地昔帕明(DMI)后PC12细胞匀浆中的结合。 PC12细胞在DMI中暴露3天可有效降低[3H]尼西西汀与NETs结合的Bmax,但不会降低KD。 [3 H]尼西汀的结合的减少取决于DMI的浓度和暴露于DMI的时间。在DMI暴露停止48小时后,[3H]尼西汀与NET的结合减少,还原为暴露前水平。当PC12细胞暴露于另一种对NET选择性药物尼索西汀时,发现NETs的类似下调,尼西汀在结构上与DMI不相关。相反,将细胞暴露于血清素转运蛋白选择性药物西酞普兰或NET底物去甲肾上腺素对[3H]尼西汀与NET的结合没有影响。 NETs的下调与完整PC12细胞中DMI诱导的[3H]去甲肾上腺素摄取减少有关。从这些数据可以推断出,NET抑制剂可以直接下调NET,并且在去甲肾上腺素的突触浓度没有变化的情况下也可以。

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