Organometallic Complexes: New Tools for Chemotherapy

Chavain, Natascha; Biot, Christophe

doi:10.2174/092986710791859306

Cited by 90 publications

(34 citation statements)

References 162 publications

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“…The methoxy groups of 1 also generated a resonance at 57.2 ppm in the 13 C NMR spectrum in acetone-d 6 All complexes were synthesized and tested as racemic mixtures of enantiomers. To demonstrate that the cyclometalated iridium(III) complexes used in this study are substitutionally inert, the stability of the complexes were investigated by 1 complexes were stable in DMSO-d 6 /D 2 O (9:1; 5 mM) at 298 K for at least seven days, as verified by 1 H NMR spectroscopy. Similarly, UV−vis absorption spectroscopy also showed that the complexes were stable in acetonitrile/Tris-HCl buffer/ (8:2; 10 μM) at 298 K for at least 7 days.…”

Section: ■ Introductionmentioning

confidence: 99%

An Iridium(III) Complex Inhibits JMJD2 Activities and Acts as a Potential Epigenetic Modulator

Liu

Zhong

et al. 2015

J. Med. Chem.

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A novel iridium(III) complex was synthesized and evaluated for its ability to target JMJD2 enzymatic activity. The iridium(III) complex 1 can inhibit JMJD2 activity and was selective for JMJD2 activity over JARID, JMJD3, and HDAC activities. Moreover, 1 suppressed the trimethylation of the p21 promoter on H3K9me3 and interrupted the JMJD2D-H3K9me3 interactions in human cells, suggesting that it could act as an epigenetic modulator. To our knowledge, 1 represents the first metal-based JMJD2 inhibitor reported in the literature.

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Section: ■ Introductionmentioning

confidence: 99%

An Iridium(III) Complex Inhibits JMJD2 Activities and Acts as a Potential Epigenetic Modulator

Liu

Zhong

et al. 2015

J. Med. Chem.

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“…But the clinical development of new compounds is often been stopped for various reasons: toxicity, chemistry, pharmacology, or economics, and less than one in ten promising molecules that have entered the pipeline reaches the stage of clinical studies. In the mid- 90 s, we extended the strategy developed by Gérard Jaouen (Vessieres et al , 1988) in anticancer therapy to antimalarial therapy (see Chavain & Biot, 2010 for review). The main antimalarials in current use (CQ, quinine, mefloquine, artemisinin, atovaquone) were modified by introduction of a ferrocenyl moiety in their chemical structure.…”

Section: The Malaria Problemmentioning

confidence: 99%

The antimalarial ferroquine: from bench to clinic

et al. 2011

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Ferroquine (FQ, SSR97193) is currently the most advanced organometallic drug candidate and about to complete phase II clinical trials as a treatment for uncomplicated malaria. This ferrocenecontaining compound is active against both chloroquine-susceptible and chloroquine-resistant Plasmodium falciparum and P. vivax strains and/or isolates. This article focuses on the discovery of FQ, its antimalarial activity, the hypothesis of its mode of action, the current absence of resistance in vitro and recent clinical trials.

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“…While it is estimated that about 70% of organic drugs are bioinspired or are derivatives of natural products, 1 putative metal-based drugs are normally synthetic. 13 Reflecting growing interest, reviews are also available describing the development of organometallic compounds as therapeutic agents [14][15][16] and, intriguingly, of metal-organic frameworks (MOFs) which may function as drug carriers, that is a new type of drug delivery system. Despite the dominance of organic molecules in chemotherapy, it is of interest that modern chemotherapy is widely acknowledged to have begun with the work of Paul Ehrlich who investigated the efficacy of arsenic compounds for the treatment of, for example, African trypanosominasis.…”

Section: Introductionmentioning

confidence: 99%