Cardioprotective effects of a novel iron chelator, pyridoxal 2-chlorobenzoyl hydrazone, in the rabbit model of daunorubicin-induced cardiotoxicity
Language English Country Netherlands Media print-electronic
Document type Journal Article, Research Support, Non-U.S. Gov't
PubMed
17003229
DOI
10.1124/jpet.106.111468
PII: S0022-3565(24)33077-0
Knihovny.cz E-resources
- MeSH
- Cell Division drug effects MeSH
- Iron Chelating Agents pharmacology MeSH
- Chinchilla MeSH
- Daunorubicin * MeSH
- Electrocardiography drug effects MeSH
- Ventricular Function, Left drug effects MeSH
- HL-60 Cells MeSH
- Hydrazones pharmacology MeSH
- Cardiotonic Agents * MeSH
- Myocardial Contraction drug effects MeSH
- Rabbits MeSH
- Blood Pressure drug effects MeSH
- Humans MeSH
- Cardiac Output drug effects MeSH
- Myocardium metabolism pathology MeSH
- Heart Diseases chemically induced pathology prevention & control MeSH
- Antibiotics, Antineoplastic * MeSH
- Pyridoxal analogs & derivatives pharmacology MeSH
- Heart Rate drug effects MeSH
- Body Weight drug effects MeSH
- Stroke Volume drug effects MeSH
- Troponin T metabolism MeSH
- Animals MeSH
- Check Tag
- Rabbits MeSH
- Humans MeSH
- Male MeSH
- Animals MeSH
- Publication type
- Journal Article MeSH
- Research Support, Non-U.S. Gov't MeSH
- Names of Substances
- Iron Chelating Agents MeSH
- Daunorubicin * MeSH
- Hydrazones MeSH
- Cardiotonic Agents * MeSH
- Antibiotics, Antineoplastic * MeSH
- pyridoxal 2-chlorobenzoyl hydrazone MeSH Browser
- Pyridoxal MeSH
- Troponin T MeSH
Iron chelation is the only pharmacological intervention against anthracycline cardiotoxicity whose effectiveness has been well documented both experimentally and clinically. In this study, we aimed to assess whether pyridoxal 2-chlorobenzoyl hydrazone (o-108, a strong iron chelator) can provide effective protection against daunorubicin (DAU)-induced chronic cardiotoxicity in rabbits. First, using the HL-60 leukemic cell line, it was shown that o-108 has no potential to blunt the antiproliferative efficacy of DAU. Instead, o-108 itself moderately inhibited cell proliferation. In vivo, chronic DAU treatment (3 mg/kg weekly for 10 weeks) induced mortality (33%), left ventricular (LV) dysfunction, a troponin T rise, and typical morphological LV damage. In contrast, all animals treated with 10 mg/kg o-108 before DAU survived without a significant drop in the LV ejection fraction (63.2 +/- 0.5 versus 59.2 +/- 1.0%, beginning versus end, not significant), and their cardiac contractility (dP/dt(max)) was significantly higher than in the DAU-only group (1131 +/- 125 versus 783 +/- 53 kPa/s, p < 0.05), which corresponded with histologically assessed lower extent and intensity of myocardial damage. Although higher o-108 dose (25 mg/kg) was well tolerated when administered alone, in combination with DAU it led to rather paradoxical and mostly negative results regarding both cardioprotection and overall mortality. In conclusion, we show that shielding of free intracellular iron using a potent lipophilic iron chelator is able to offer a meaningful protection against chronic anthracycline cardiotoxicity. However, this approach lost its potential with the higher chelator dose, which suggests that iron might play more complex role in the pathogenesis of this disease than previously assumed.
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