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  4. Exploring metallodrug-protein interactions by mass spectrometry: comparisons between platinum coordination complexes and an organometallic ruthenium compound
 
research article

Exploring metallodrug-protein interactions by mass spectrometry: comparisons between platinum coordination complexes and an organometallic ruthenium compound

Casini, Angela  
•
Gabbiani, Chiara
•
Michelucci, Elena
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2009
JBIC, JOURNAL OF BIOLOGICAL INORGANIC CHEMISTRY

Electrospray ionisation mass spectrometry was used to analyze the reactions of metal compds. with mixts. of selected proteins. Three representative medicinally relevant compds., cisplatin, transplatin and the organometallic ruthenium compd. RAPTA-C, were reacted with a pool of three proteins, ubiquitin, cytochrome c and superoxide dismutase, and the reaction products were analyzed using high-resoln. mass spectrometry. Highly informative electrospray ionisation mass spectra were acquired following careful optimization of the exptl. conditions. The formation of metal-protein adducts was clearly obsd. for the three proteins. In addn., valuable information was obtained on the nature of the protein-bound metallofragments, on their distribution among the three different proteins and on the binding kinetics. The platinum compds. were less reactive and considerably less selective in protein binding than RAPTA-C, which showed a high affinity towards ubiquitin and cytochrome c, but not superoxide dismutase. In addn., competition studies between cisplatin and RAPTA-C showed that the two metallodrugs have affinities for the same amino acid residues on protein binding.

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Type
research article
DOI
10.1007/s00775-009-0489-5
Web of Science ID

WOS:000266924400012

Author(s)
Casini, Angela  
Gabbiani, Chiara
Michelucci, Elena
Pieraccini, Giuseppe
Moneti, Gloriano
Dyson, Paul J.  
Messori, Luigi
Date Issued

2009

Publisher

Springer-Verlag

Published in
JBIC, JOURNAL OF BIOLOGICAL INORGANIC CHEMISTRY
Volume

14

Issue

5

Start page

761

End page

770

Subjects

Cisplatin

•

Metal-based drugs

•

Proteins

•

Bioorganometallic chemistry

•

Mechanism of action

•

Heart Cytochrome-C

•

Anticancer Drugs

•

Esi-Ms

•

Binding-Sites

•

Liquid-Chromatography

•

Gold(Iii) Compounds

•

Breast-Cancer

•

Dna

•

Cisplatin

•

Mechanisms

Note

National Licences

Editorial or Peer reviewed

REVIEWED

Written at

EPFL

EPFL units
LCOM  
Available on Infoscience
April 6, 2010
Use this identifier to reference this record
https://infoscience.epfl.ch/handle/20.500.14299/49151
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