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Literature DB >> 21151827

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

Michael Groessl¹, Mattia Terenghi, Angela Casini, Lisa Elviri, Ryszard Lobinski, Paul J Dyson.

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.

Entities: Chemical Disease Gene Species

Year: 2010 PMID： 21151827 PMCID： PMC2999900 DOI： 10.1039/B922701F

Source DB: PubMed Journal: J Anal At Spectrom ISSN： 0267-9477 Impact factor: 4.023

41 in total

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6. Characterisation of cisplatin coordination sites in cellular Escherichia coli DNA-binding proteins by combined biphasic liquid chromatography and ESI tandem mass spectrometry.

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7. Characterisation of cisplatin binding sites in human serum proteins using hyphenated multidimensional liquid chromatography and ESI tandem mass spectrometry.

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8. Capillary electrophoresis hyphenated to inductively coupled plasma-mass spectrometry: a novel approach for the analysis of anticancer metallodrugs in human serum and plasma.

Authors: Michael Groessl; Christian G Hartinger; Kasia Polec-Pawlak; Maciej Jarosz; Bernhard K Keppler
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Review 9. The synergy of elemental and biomolecular mass spectrometry: new analytical strategies in life sciences.

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10. Platinum metallodrug-protein binding studies by capillary electrophoresis-inductively coupled plasma-mass spectrometry: characterization of interactions between Pt(II) complexes and human serum albumin.

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3. Competitive binding of Fe3+, Cr3+, and Ni2+ to transferrin.

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Journal: J Biol Inorg Chem Date: 2011-06-17 Impact factor: 3.358

4. The interactions of the ruthenium(II)-cymene complexes with lysozyme and cytochrome c.

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5. Comparative in vitro and in vivo pharmacological investigation of platinum(IV) complexes as novel anticancer drug candidates for oral application.

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6. The impact of whole human blood on the kinetic inertness of platinum(iv) prodrugs - an HPLC-ICP-MS study.

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7. Target profiling of an antimetastatic RAPTA agent by chemical proteomics: relevance to the mode of action.

Authors: Maria V Babak; Samuel M Meier; Kilian V M Huber; Jóhannes Reynisson; Anton A Legin; Michael A Jakupec; Alexander Roller; Alexey Stukalov; Manuela Gridling; Keiryn L Bennett; Jacques Colinge; Walter Berger; Paul J Dyson; Giulio Superti-Furga; Bernhard K Keppler; Christian G Hartinger
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8. Critical assessment of different methods for quantitative measurement of metallodrug-protein associations.

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Review 9. Metallodrugs are unique: opportunities and challenges of discovery and development.

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10. Systemic administration of 3-bromopyruvate reveals its interaction with serum proteins in a rat model.

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Journal: BMC Res Notes Date: 2013-07-17