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AGP 的糖基化及其与美沙酮结合的关系。

The glycosylation of AGP and its associations with the binding to methadone.

机构信息

School of Life, Sport and Social Sciences, Edinburgh Napier University, Sighthill Campus, Edinburgh, UK.

出版信息

Biomed Res Int. 2013;2013:108902. doi: 10.1155/2013/108902. Epub 2013 Jul 15.

Abstract

Methadone remains the most common form of pharmacological therapy for opioid dependence; however, there is a lack of explanation for the reports of its relatively low success rate in achieving complete abstinence. One hypothesis is that in vivo binding of methadone to the plasma glycoprotein alpha-1-acid glycoprotein (AGP), to a degree dependent on the molecular structure, may render the drug inactive. This study sought to determine whether alterations present in the glycosylation pattern of AGP in patients undergoing various stages of methadone therapy (titration < two weeks, harm reduction < one year, long-term > one and a half years) could affect the affinity of the glycoprotein to bind methadone. The composition of AGP glycosylation was determined using high pH anion exchange chromatography (HPAEC) and intrinsic fluorescence analysed to determine the extent of binding to methadone. The monosaccharides galactose and N-acetyl-glucosamine were elevated in all methadone treatment groups indicating alterations in AGP glycosylation. AGP from all patients receiving methadone therapy exhibited a greater degree of binding than the normal population. This suggests that analysing the glycosylation of AGP in patients receiving methadone may aid in determining whether the therapy is likely to be effective.

摘要

美沙酮仍然是治疗阿片类药物依赖的最常见的药物治疗形式;然而,对于其实现完全戒断的相对低成功率的报告,缺乏解释。一种假设是,美沙酮在体内与血浆糖蛋白α-1-酸性糖蛋白(AGP)结合,在一定程度上取决于分子结构,可能使药物失活。本研究旨在确定接受美沙酮治疗的各个阶段(滴定<两周,减少危害<一年,长期>一年半)的患者的 AGP 糖基化模式的改变是否会影响糖蛋白与美沙酮结合的亲和力。使用高 pH 阴离子交换色谱(HPAEC)测定 AGP 的糖基化组成,并分析内在荧光以确定与美沙酮结合的程度。所有美沙酮治疗组的半乳糖和 N-乙酰葡萄糖胺单糖升高,表明 AGP 糖基化发生改变。所有接受美沙酮治疗的患者的 AGP 表现出比正常人群更高的结合程度。这表明分析接受美沙酮治疗的患者的 AGP 糖基化可能有助于确定治疗是否可能有效。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/3f5e/3727094/bf28f46e26d0/BMRI2013-108902.001.jpg

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