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research article

Development of Ruthenium Antitumor Drugs that Overcome Multidrug Resistance Mechanisms

Vock, CA  
•
Ang, WH  
•
Scolaro, C  
Show more
2007
JOURNAL OF MEDICINAL CHEMISTRY

Organometallic ruthenium(II) complexes of the general formula [Ru(η<SUP>6</SUP>-<I>p</I>-cymene)Cl<SUB>2</SUB>(L)] and [Ru(η<SUP>6</SUP>-<I>p</I>-cymene)Cl(L)<SUB>2</SUB>][BPh<SUB>4</SUB>] with modified phenoxazine- and anthracene-based multidrug resistance (MDR) modulator ligands (L) have been synthesized, spectroscopically characterized, and evaluated in vitro for their cytotoxic and MDR reverting properties in comparison with the free ligands. For an anthracene-based ligand, coordination to a ruthenium(II) arene fragment led to significant improvement of cytotoxicity as well as Pgp inhibition activity. A similar, but weaker effect was also observed when using a benzimidazole-phenoxazine derivative as Pgp inhibitor. The most active compound in terms of both Pgp inhibition and cytotoxicity is [Ru(η<SUP>6</SUP>-<I>p</I>-cymene)Cl<SUB>2</SUB>(L)], where L is an anthracene-based ligand. Studies show that it induces cell death via inhibition of DNA synthesis. Moreover, because the complex is fluorescent, its uptake in cells was studied, and relative to the free anthracene-based ligand, uptake of the complex is accelerated and accumulation of the complex in the cell nucleus is observed.

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Type
research article
DOI
10.1021/jm070039f
Web of Science ID

WOS:000245954600019

Author(s)
Vock, CA  
Ang, WH  
Scolaro, C  
Phillips, AD  
Lagopoulos, L
Juillerat-Jeanneret, L
Sava, G
Scopelliti, R  
Dyson, PJ  
Date Issued

2007

Published in
JOURNAL OF MEDICINAL CHEMISTRY
Volume

50

Issue

9

Start page

2166

End page

2175

Editorial or Peer reviewed

REVIEWED

Written at

EPFL

EPFL units
LCOM  
Available on Infoscience
June 13, 2007
Use this identifier to reference this record
https://infoscience.epfl.ch/handle/20.500.14299/7891
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