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糖基化和脂肪酸引起的磺酰脲类药物与人血清白蛋白结合变化的色谱研究。

Chromatographic studies of changes in binding of sulfonylurea drugs to human serum albumin due to glycation and fatty acids.

机构信息

Chemistry Department, University of Nebraska, Lincoln, Lincoln, NE 68588-0304, USA.

出版信息

J Chromatogr B Analyt Technol Biomed Life Sci. 2010 Nov 15;878(30):3193-7. doi: 10.1016/j.jchromb.2010.09.033. Epub 2010 Oct 23.

Abstract

This report examines the use of high-performance affinity chromatography as a screening tool for studying the change in binding by sulfonylurea drugs to the protein human serum albumin (HSA) during diabetes. The effects of both the non-enzymatic glycation of HSA and the presence of fatty acids on these interactions were considered using a zonal elution format. It was found that there was a significant increase (i.e., 2.7- to 3.6-fold) in the relative retention of several sulfonylurea drugs (i.e., acetohexamide, tolbutamide, glybenclamide and gliclazide) on columns containing normal versus glycated HSA. The addition of various long chain fatty acids to the mobile phase gave the same trend in retention for the tested drugs on both the HSA and glycated HSA columns, generally leading to lower binding. Most of the fatty acids examined produced similar or moderately different relative shifts in retention; however, palmitic acid was found to produce a much larger change in retention on columns containing glycated HSA versus normal HSA under the conditions used in this study.

摘要

本报告探讨了使用高效亲和色谱作为筛选工具,研究磺酰脲类药物与蛋白质人血清白蛋白(HSA)结合的变化,以在糖尿病期间发生这种变化。使用区带洗脱格式考虑了 HSA 的非酶糖基化和脂肪酸存在对这些相互作用的影响。结果发现,与包含正常 HSA 的柱相比,几种磺酰脲类药物(即醋磺己脲、甲苯磺丁脲、格列本脲和格列齐特)在包含糖基化 HSA 的柱上的相对保留时间显著增加(即 2.7-3.6 倍)。向流动相中添加各种长链脂肪酸会导致在 HSA 和糖基化 HSA 柱上测试药物的保留时间呈现相同的趋势,通常导致结合减少。在所研究的条件下,大多数检查的脂肪酸在保留时间上产生相似或略有不同的相对位移;然而,与在正常 HSA 柱相比,棕榈酸在包含糖基化 HSA 的柱上导致的保留时间变化要大得多。

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