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首页> 外文OA文献 >The Drug of Abuse γ-Hydroxybutyrate Is a Substrate for Sodium-Coupled Monocarboxylate Transporter (SMCT) 1 (SLC5A8): Characterization of SMCT-Mediated Uptake and Inhibition
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The Drug of Abuse γ-Hydroxybutyrate Is a Substrate for Sodium-Coupled Monocarboxylate Transporter (SMCT) 1 (SLC5A8): Characterization of SMCT-Mediated Uptake and Inhibition

机译:滥用药物γ-羟基丁酸酯是药物的底物 钠耦合的单羧酸盐转运蛋白(SMCT)1(SLC5A8):表征 介导的CTCT摄取和抑制

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摘要

γ-Hydroxybutyric acid (GHB), a drug of abuse, is a substrate of monocarboxylate transporters (MCTs). Sodium-coupled monocarboxylate transporter 1 (SMCT1; SLC5A8) is expressed in kidney, thyroid gland, neurons, and intestinal tract and exhibits substrate specificity similar to that of the proton-dependent MCT (SLC16A) family. The role of SMCT1 in GHB disposition has not been determined. In this study we characterized the driving force, transport kinetics, and inhibitors of GHB uptake, as well as expression of SMCT and MCT isoforms, in rat thyroid follicular (FRTL-5) cells. GHB, as well as the monocarboxylates butyrate and d-lactate, exhibited sodium-dependent uptake at pH 7.4, which could be described with a simple Michaelis-Menten equation plus a diffusional component [Km 0.68 ± 0.30 mM, Vmax 3.50 ± 1.58 nmol · mg–1 · min–1, and diffusional clearance (P) 0.25 ± 0.08 μl · mg–1 · min–1]. In the absence of sodium, GHB uptake was significantly increased at lower pH, suggesting proton-gradient dependent transport. Reverse transcriptase-polymerase chain reaction and Western analyses demonstrated the expression of SMCT1, MCT1, and MCT2 in FRTL-5 cells, supporting the activity results. Sodium-dependent GHB uptake in FRTL-5 cells was inhibited by MCT substrates (d-lactate, l-lactate, pyruvate, and butyrate), nonsteroidal anti-inflammatory drugs (ibuprofen, ketoprofen, and naproxen), and probenecid. IC50 values for l-lactate, ibuprofen, ketoprofen, and probenecid were 101, 31.6, 64.4, and 380 μM, respectively. All four inhibitors also significantly inhibited GHB uptake in rat MCT1 gene-transfected MDA/MB231 cells, suggesting they are not specific for SMCT1. Luteolin and α-cyano-4-hydroxycinnimate represent specific proton-dependent MCT inhibitors. Our findings indicate that GHB is a substrate for both sodium- and proton-dependent MCTs and identified specific inhibitors of MCTs.
机译:γ-羟基丁酸(GHB)是一种滥用药物,是单羧酸盐转运蛋白(MCT)的底物。钠偶联的单羧酸盐转运蛋白1(SMCT1; SLC5A8)在肾脏,甲状腺,神经元和肠道中表达,并表现出与质子依赖性MCT(SLC16A)家族相似的底物特异性。尚未确定SMCT1在GHB处置中的作用。在这项研究中,我们表征了大鼠甲状腺滤泡(FRTL-5)细胞中GHB摄取的驱动力,转运动力学和抑制剂,以及SMCT和MCT亚型的表达。 GHB以及丁酸单羧酸酯和d-乳酸在pH 7.4时表现出钠依赖性的吸收,这可以用一个简单的Michaelis-Menten方程加一个扩散成分来描述[Km 0.68±0.30 mM,Vmax 3.50±1.58 nmol· mg-1·min-1,扩散清除率(P)0.25±0.08μl·mg-1·min-1]。在没有钠的情况下,在较低的pH值下,GHB的摄取显着增加,表明质子梯度依赖性转运。逆转录聚合酶链反应和Western分析表明FRTL-5细胞中SMCT1,MCT1和MCT2的表达,支持了活性结果。 MCT底物(d-乳酸,l-乳酸,丙酮酸和丁酸),非甾体抗炎药(布洛芬,酮洛芬和萘普生)和丙磺舒抑制了FRTL-5细胞中钠依赖性GHB的吸收。乳酸,布洛芬,酮洛芬和丙磺舒的IC50值分别为101、31.6、64.4和380μM。所有这四种抑制剂也都显着抑制了大鼠MCT1基因转染的MDA / MB231细胞中GHB的摄取,表明它们对SMCT1不是特异性的。木犀草素和α-氰基-4-羟基肉桂酸酯代表特定的质子依赖性MCT抑制剂。我们的发现表明,GHB是钠依赖性和质子依赖性MCT的底物,并且已鉴定出MCT的特异性抑制剂。

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