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Single nucleotide polymorphisms of ABCC2 modulate renal secretion of endogenous organic anions

机译:ABCC2的单核苷酸多态性调节内源性有机阴离子的肾分泌

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Graphical abstract Display Omitted Abstract The ATP-binding cassette family transporter MRP2 (multidrug resistance-associated protein 2), encoded by the ABCC2 gene, is involved in the renal excretion of numerous xenobiotics and it is likely that it also transports many endogenous molecules arising from not only normal essential metabolic processes but also from environmental toxins or food intake. We used a targeted gas chromatography-mass spectrometry metabolomics analysis to study whether endogenous organic anions are differentially excreted in urines of healthy volunteers according to their genotype for three functional single nucleotide polymorphisms (SNPs) in ABCC2 . This was the case for 35 of the 108 metabolites analyzed. Eight of them are most likely substrates of MRP2 since they are the most contributive to the difference between carriers of a decreasing function allele vs those carrying an increasing function one. Seven out of 8 metabolites are fatty acids (dodecanoic acid; 3-hydroxypropanoic acid) or metabolites of polyphenols (caffeine; resorcinol; caffeic acid; 2-(3,4-dihydroxyphenyl) acetic acid; and 4-hydroxyhippuric acid). Most of them were structurally similar to a series of substances previously shown to interact with MRP2 function in vitro. Interestingly, coproporphyrin isomer I, a prototypical substrate of MRP2, also belonged to our final list although it was not significantly discriminant on its own. This suggests that the simultaneous measurement of a set of endogenous metabolites in urine, rather than that of unique metabolites, has the potential to provide a phenotypic measure of MRP2 function in vivo . This would represent an innovative tool to study the variability of the transport activity of MRP2 under a physiological or pathological condition, especially in pharmacokinetic studies of its substrates. ]]>
机译:摘要摘要摘要摘要ABCC2基因编码的ATP结合盒系列转运蛋白MRP2(多药抗性相关蛋白2)参与了许多异种症的肾脏排泄,并且它可能还运于许多内源分子不仅是正常的基本代谢过程,还来自环境毒素或食物摄入量。我们使用了靶向气相色谱 - 质谱法代谢组科分析来研究内源性有机阴离子是否根据其在ABCC2中的三种功能单核苷酸多态性(SNP)的基因型在健康志愿者的尿中差异排出。对于分析的108种代谢物中的35例,这是这种情况。其中八个是MRP2的最有可能的基质,因为它们是携带增加函数的函数等位基因的载流子之间的差异的最大贡献。 8种代谢物中的七种是脂肪酸(十二烷酸; 3-羟基丙酸)或多酚代谢物(咖啡因;间苯二酚;咖啡酸; 2-(3,4-二羟基苯基)乙酸;和4-羟基尿酸)。它们中的大多数是在结构上类似于先前所示的一系列物质与体外与MRP2功能相互作用的物质。有趣的是,Coproporphyrin异构体I,MRP2的原型底物也属于我们的最终名单,尽管它并没有自行判别。这表明尿液中一组内源性代谢物的同时测量,而不是独特的代谢物,具有潜力在体内提供MRP2功能的表型测量。这将代表一种创新工具,用于研究MRP2在生理或病理条件下的运输活性的可变性,特别是在其基材的药代动力学研究中。 ]]>

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