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双氯芬酸药物与一组中度糖化血清白蛋白结合的量热法研究。

Calorimetric investigation of diclofenac drug binding to a panel of moderately glycated serum albumins.

作者信息

Indurthi Venkata S K, Leclerc Estelle, Vetter Stefan W

机构信息

Department of Pharmaceutical Sciences, North Dakota State University Fargo, ND, USA.

出版信息

Eur J Pharm Sci. 2014 Aug 1;59:58-68. doi: 10.1016/j.ejps.2014.04.002. Epub 2014 Apr 19.

DOI:10.1016/j.ejps.2014.04.002
PMID:24751671
Abstract

Glycation alters the drug binding properties of serum proteins and could affect free drug concentrations in diabetic patients with elevated glycation levels. We investigated the effect of bovine serum albumin glycation by eight physiologically relevant glycation reagents (glucose, ribose, carboxymethyllysine, acetoin, methylglyoxal, glyceraldehyde, diacetyl and glycolaldehyde) on diclofenac drug binding. We used this non-steroidal anti-inflammatory drug diclofenac as a paradigm for acidic drugs with high serum binding and because of its potential cardiovascular risks in diabetic patients. Isothermal titration calorimetry showed that glycation reduced the binding affinity Ka of serum albumin and diclofenac 2 to 6-fold by reducing structural rigidity of albumin. Glycation affected the number of drug binding sites in a glycation reagent dependent manner and lead to a 25% decrease for most reagent, expect for ribose, with decreased by 60% and for the CML-modification, increased the number of binding sites by 60%. Using isothermal titration calorimetry and differential scanning calorimetry we derived the complete thermodynamic characterization of diclofenac binding to all glycated BSA samples. Our results suggest that glycation in diabetic patients could significantly alter the pharmacokinetics of the widely used over-the-counter NSDAI drug diclofenac and with possibly negative implications for patients.

摘要

糖基化会改变血清蛋白的药物结合特性,并可能影响糖化水平升高的糖尿病患者的游离药物浓度。我们研究了八种生理相关糖基化试剂(葡萄糖、核糖、羧甲基赖氨酸、乙偶姻、甲基乙二醛、甘油醛、双乙酰和乙醇醛)对牛血清白蛋白糖基化后双氯芬酸药物结合的影响。我们使用这种非甾体抗炎药双氯芬酸作为高血清结合酸性药物的范例,并且因为它在糖尿病患者中有潜在的心血管风险。等温滴定量热法表明,糖基化通过降低白蛋白的结构刚性,使血清白蛋白与双氯芬酸的结合亲和力Ka降低了2至6倍。糖基化以糖基化试剂依赖的方式影响药物结合位点的数量,大多数试剂导致结合位点数量减少25%,核糖除外,其减少了60%,而羧甲基赖氨酸修饰则使结合位点数量增加了60%。使用等温滴定量热法和差示扫描量热法,我们得出了双氯芬酸与所有糖基化牛血清白蛋白样品结合的完整热力学特征。我们的结果表明,糖尿病患者的糖基化可能会显著改变广泛使用的非处方非甾体抗炎药双氯芬酸的药代动力学,并可能对患者产生负面影响。

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