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Top-Down Mass Spectrometric Approach for the Full Characterization of Insulin-Cisplatin Adducts

机译:胰岛素-顺铂加合物的完整表征的自顶向下质谱方法

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The interaction of the antitumor drug cisplatin with insulin was studied using a top-down mass spectrometric approach. In vitro incubations were prepared under acidic and physiological conditions at different insulin/cisplatin molar ratios for different incubation times. Size exclusion chromatography-inductively coupled plasma mass spectrometry (SEC-ICPMS) analysis enabled the specific detection of platinum containing species attributed to the binding of the drug to the protein. Further analysis through matrix-assisted laser desorption ionization-time-of-flight mass spectrometry (MALDI-TOF MS) and nanoelectrospray ionization mass spectrometry using a linear ion trap (nESI-LIT-MS) allowed the identification of platinated mono-, di-, and even triadducts in the incubations. Platinum binding sites were identified by CID-MS~(n) as B chain N-terminus, His5, and probably His10 residues, which turned out to be the same, regardless of the incubation conditions. Evidence on the binding of Pt to B chain Cys7 was also observed. Working with the LIT zoom scan mode provides enough resolution to discern the isotopic pattern for both precursor and fragment ions, allowing the differentiation of platinum-containing ions. The elucidation of platinum binding sites in a native protein through a top-down approach has been performed for the first time with this type of instrument.
机译:使用自上而下的质谱方法研究了抗肿瘤药顺铂与胰岛素的相互作用。在不同的孵育时间下,在酸性和生理条件下以不同的胰岛素/顺铂摩尔比制备体外孵育。尺寸排阻色谱-电感耦合等离子体质谱(SEC-ICPMS)分析能够特异性检测归因于药物与蛋白质结合的含铂物质。通过基质辅助激光解吸电离飞行时间质谱(MALDI-TOF MS)和使用线性离子阱(nESI-LIT-MS)的纳米电喷雾电离质谱的进一步分析,可以鉴定出镀铂的单,双,甚至是孵化中的三加合物。通过CID-MS〜(n)将铂结合位点鉴定为B链N端,His5以及可能的His10残基,无论孵育条件如何,结果均相同。还观察到Pt与B链Cys7结合的证据。使用LIT缩放扫描模式可提供足够的分辨率,以辨别前体离子和碎片离子的同位素模式,从而区分含铂离子。这类仪器首次通过自上而下的方法阐明了天然蛋白质中的铂结合位点。

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