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抗癌金属药物与血清蛋白的反应性:尺寸排阻色谱-电感耦合等离子体质谱和电喷雾电离质谱的新见解

Reactivity of anticancer metallodrugs with serum proteins: new insights from size exclusion chromatography-ICP-MS and ESI-MS.

作者信息

Groessl Michael, Terenghi Mattia, Casini Angela, Elviri Lisa, Lobinski Ryszard, Dyson Paul J

机构信息

Institut des Sciences et Ingénierie Chimiques, Ecole Polytechnique Fédérale de Lausanne (EPFL), CH-1015 Lausanne, Switzerland.

出版信息

J Anal At Spectrom. 2010 Mar;25(3):305-313. doi: 10.1039/B922701F.

Abstract

A method based on the coupling of high resolution size-exclusion liquid chromatography using a polymer stationary phase with inductively coupled plasma mass spectrometry was developed to study the interactions of two metallodrugs - cisplatin and RAPTA-T - with the serum proteins albumin and transferrin. In contrast to previous approaches, the technique allowed the total recovery of the metals from the column and was able to discriminate between the different species of the metallodrugs and their complexes with the proteins at femtomolar detection levels. Metal binding was found to be dependent on the protein concentration and on the incubation time of the sample. Cisplatin was found to bind the serum proteins to the same extent, whereas RAPTA-T showed marked preference for transferrin. The affinity of the ruthenium complex for holo-transferrin was higher than for the apo-form suggesting a cooperative iron-mediated metal binding mechanism. RAPTA-T binding to holo-transferrin was further investigated by electrospray mass spectrometry using both the intact protein and a model peptide mimicking the iron-binding pocket.

摘要

开发了一种基于使用聚合物固定相的高分辨率尺寸排阻液相色谱与电感耦合等离子体质谱联用的方法,以研究两种金属药物——顺铂和RAPTA-T——与血清蛋白白蛋白和转铁蛋白的相互作用。与先前的方法不同,该技术能够从柱中完全回收金属,并且能够在飞摩尔检测水平上区分金属药物的不同种类及其与蛋白质的复合物。发现金属结合取决于蛋白质浓度和样品的孵育时间。发现顺铂与血清蛋白的结合程度相同,而RAPTA-T对转铁蛋白表现出明显的偏好。钌配合物对全转铁蛋白的亲和力高于对脱辅基形式的亲和力,表明存在协同铁介导的金属结合机制。使用完整蛋白质和模拟铁结合口袋的模型肽,通过电喷雾质谱进一步研究了RAPTA-T与全转铁蛋白的结合。

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