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Molecular and functional characterization of riboflavin specific transport system in rat brain capillary endothelial cells

机译:大鼠脑毛细管内皮细胞中核黄素特异性运输系统的分子与功能性

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摘要

Riboflavin is an important water soluble vitamin (B2) required for metabolic reactions, normal cellular growth, differentiation and function. Mammalian brain cells cannot synthesize riboflavin and must import from systemic circulation. However, the uptake mechanism, cellular translocation and intracellular trafficking of riboflavin in brain capillary endothelial cells are poorly understood. The primary objective of this study is to investigate the existence of riboflavin-specific transport system and delineate the uptake and intracellular regulation of riboflavin in immortalized rat brain capillary endothelial cells (RBE4). The uptake of [3H]-Riboflavin is sodium, temperature and energy dependent but pH independent. [3H]-Riboflavin uptake is saturable with Km and Vmax values of 19 ± 3 µM and 0.235 ± 0.012 picomoles/min/mg protein, respectively. The uptake process is inhibited by unlabelled structural analogs (lumiflavin, lumichrome) but not by structurally unrelated vitamins. Ca++/calmodulin and protein kinase A (PKA) pathways are found to play an important role in the intracellular regulation of [3H]-Riboflavin. Apical and baso-lateral uptake of [3H]-Riboflavin clearly indicate that riboflavin specific transport system is predominantly localized on the apical side of RBE4 cells. A 628 bp band corresponding to riboflavin transporter is revealed in RT-PCR analysis. These findings, for the first time report the existence of a specialized and high affinity transport system for riboflavin in RBE4 cells. Blood-brain barrier (BBB) is a major obstacle limiting drug transport inside the brain as it regulates drug permeation from systemic circulation. This transporter can be utilized for targeted delivery in enhancing brain permeation of highly potent drugs on systemic administration.
机译:Riboflavin是代谢反应,正常细胞生长,分化和功能所需的重要水溶性维生素(B2)。哺乳动物脑细胞不能合成核黄素,必须从系统性循环中导入。然而,脑毛细管内皮细胞中核黄素的摄取机制,细胞易位和细胞内运输差不多。本研究的主要目的是探讨核黄素特异性运输系统的存在,并描绘核黄素在永生大鼠脑毛细管内皮细胞(RBE4)中的核黄素摄取和细胞内调节。 [3H] -1Riboflavin的吸收是钠,温度和能量依赖性,但依赖于pH独立。 [3H] -1Riboflavin吸收可饱和Km和Vmax值,分别为19±3μm和0.235±0.012皮质摩托/ min / mg蛋白质。通过未标记的结构类似物(Lumiflavin,Lumichrome)抑制摄取过程,但不是通过结构不相关的维生素。 Ca ++ / calmodulin和蛋白激酶a(pka)途径在[3h] -1riboflavin的细胞内调节中起重要作用。 [3H] -1Riboflavin的顶端和碱横向摄取清楚地表明,核黄素特异性运输系统主要归入RBE4细胞的顶端侧。在RT-PCR分析中揭示了对应于核黄素转运蛋白转运蛋白的628bp带。这些发现首次报告了RBE4细胞中核黄素的专用和高亲和传输系统的存在。血脑屏障(BBB)是脑内的主要障碍,因为它调节从系统性循环中的药物渗透性。该转运物可用于靶向递送,以提高高效药物对全身施用的高效药物渗透。

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