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首页> 外文期刊>Journal of Neurochemistry: Offical Journal of the International Society for Neurochemistry >The Na+-dependent L-ascorbic acid transporter SVCT2 expressed in brainstem cells, neurons, and neuroblastoma cells is inhibited by flavonoids.
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The Na+-dependent L-ascorbic acid transporter SVCT2 expressed in brainstem cells, neurons, and neuroblastoma cells is inhibited by flavonoids.

机译:黄酮类化合物抑制在脑干细胞,神经元和神经母细胞瘤细胞中表达的Na +依赖性L-抗坏血酸转运蛋白SVCT2。

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Ascorbic acid (AA) is best known for its role as an essential nutrient in humans and other species. As the brain does not synthesize AA, high levels are achieved in this organ by specific uptake mechanisms, which concentrate AA from the bloodstream to the CSF and from the CSF to the intracellular compartment. Two different isoforms of sodium-vitamin C co-transporters (SVCT1 and SVCT2) have been cloned. Both SVCT proteins mediate high affinity Na(+)-dependent L-AA transport and are necessary for the uptake of vitamin C in many tissues. In the adult brain the expression of SVCT2 was observed in the hippocampus and cortical neurons by in situ hybridization; however, there is no data regarding the expression and distribution of this transporter in the fetal brain. The expression of SVCT2 in embryonal mesencephalic neurons has been shown by RT-PCR suggesting an important role for vitamin C in dopaminergic neuronal differentiation. We analyze SVCT2 expression in human and rat developing brain by RT-PCR. Additionally, we study the normal localization of SVCT2 in rat fetal brain by immunohistochemistry and in situ hybridization demonstrating that SVCT2 is highly expressed in the ventricular and subventricular area of the rat brain. SVCT2 expression and function was also confirmed in neurons isolated from brain cortex and cerebellum. The kinetic parameters associated with the transport of AA in cultured neurons and neuroblastoma cell lines were also studied. We demonstrate two different affinity transport components for AA in these cells. Finally, we show the ability of different flavonoids to inhibit AA uptake in normal or immortalized neurons. Our data demonstrates that brain cortex and cerebellar stem cells, neurons and neuroblastoma cells express SVCT2. Dose-dependent inhibition analysis showed that quercetin inhibited AA transport in cortical neurons and Neuro2a cells.
机译:抗坏血酸(AA)作为人类和其他物种的必需营养素而闻名。由于大脑不合成AA,因此通过特定的摄取机制在该器官中达到高水平,该机制将AA从血流集中到CSF,再从CSF集中到细胞内。已克隆了钠-维生素C共转运蛋白的两种不同同工型(SVCT1和SVCT2)。两种SVCT蛋白都介导高亲和力的Na(+)依赖型L-AA转运,并且对于许多组织中的维生素C吸收是必需的。在成年大脑中,通过原位杂交在海马和皮质神经元中观察到了SVCT2的表达。但是,没有关于该转运蛋白在胎儿脑中表达和分布的数据。 RT-PCR已显示SVCT2在胚胎中脑神经元中的表达,表明维生素C在多巴胺能神经元分化中具有重要作用。我们通过RT-PCR分析了SVCT2在人类和大鼠大脑发育中的表达。此外,我们通过免疫组织化学和原位杂交研究了SVCT2在大鼠胎脑中的正常定位,表明SVCT2在大鼠脑室和脑室下区域高度表达。在从大脑皮层和小脑分离的神经元中也证实了SVCT2的表达和功能。还研究了与AA在培养的神经元和神经母细胞瘤细胞系中运输相关的动力学参数。我们展示了在这些细胞中AA的两种不同的亲和转运成分。最后,我们显示了不同的类黄酮抑制正常或永生化神经元吸收AA的能力。我们的数据表明,大脑皮层和小脑干细胞,神经元和神经母细胞瘤细胞表达SVCT2。剂量依赖性抑制分析表明,槲皮素抑制了皮质神经元和Neuro2a细胞中的AA转运。

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