Antiproliferative and iron chelating efficiency of the new bis-8-hydroxyquinoline benzylamine chelator S1 in hepatocyte cultures

Lescoat, Gérard; Léonce, Stéphane; Pierre, Alain; Gouffier, Lucie; Gaboriau, François

Antiproliferative and iron chelating efficiency of the new bis-8-hydroxyquinoline benzylamine chelator S1 in hepatocyte cultures

2012

Lescoat, Gérard | Léonce, Stéphane | Pierre, Alain | Gouffier, Lucie | Gaboriau, François

If a new generation of iron chelators specifically devoted for cancer chemotherapy emerged these last years, any of them has not yet been approved at this time. Accordingly, there is a need to optimize new chelating molecules for iron chelation therapy and cancer treatment. So, the objective of the present investigation was to characterize the antiproliferative activity and the iron chelating capacity of the iron chelator S1 [bis-N-(8-hydroxyquinoline-5-ylmethyl)benzylamine]. Its effects were compared to O-trensox which binds ferric iron with a very high affinity (pFe³⁺=29.5). For this purpose, primary rat hepatocyte stimulated by EGF and human hepatoma HepaRG cell cultures were used. In these models, the anti-proliferative effect, the inhibition of DNA synthesis and the iron-chelating efficiency of increasing concentrations of S1 and O-trensox (0 up to 200μM) were investigated. In the two cell culture models, we observed that S1 was about 100 times more efficient than O-trensox and the antiproliferative effect of S1 in HepaRG cells appeared at concentrations as low as 0.1μM without cytotoxicity. Moreover, the stoichiometry of S1 for iron seemed to be in the range S1/Fe³⁺=1. Using the calcein fluorescence assay, we demonstrated that the affinity of S1 for iron was better than that of O-trensox since it was at least two times more effective to restore the fluorescence of calcein previously quenched by iron. So, the iron chelating efficiency of S1 could explain at least partially its higher anti-proliferative effect compared to O-trensox. Finally, these results suggest that molecules such as S1 may constitute a promising starting point to improve cancer treatment.

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AGROVOC Keywords

animals carcinoma cell culture chelating agents chelation chemical synthesis chemistry chemotherapy cytotoxicity dna drug therapy fluorescence humans humans iron metabolism models pathology pharmacology rats rats rats toxicity tests

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Published in

Chemico-biological interactions

Volume 195 Issue 2 Pagination 165 - 172 ISSN 0009-2797

Publisher

Elsevier Ireland Ltd

Other Subjects

Drug effects; Hepatoma; Ethylamines; Hydroxyquinolines; Iron chelating agents; Benzylamines; Drug; Dose-response relationship; Hepatocellular; Analogs & derivatives; Cell proliferation; Male; Oxyquinoline; Stoichiometry; Hepatocytes; Sprague-dawley

Language

English

Note

2019-12-06

Type

Journal Article; Text

In AGRIS since: 2024-02-28

Format: MODS

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DOI DOI http://dx.doi.org/10.1016/j.cbi.2011.12.003

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Antiproliferative and iron chelating efficiency of the new bis-8-hydroxyquinoline benzylamine chelator S1 in hepatocyte cultures

2012

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