Epothilones are a novel class of microtubule-targeting anticancer agents that have a similar mechanism of action to the taxanes (i.e. polymerization of tubulin dimers into microtubules and stabilization of preformed microtubules) but show antiproliferative activity in taxane-resistant tumor cells. In order to study the epothilone B (EpoB)-induced neurotoxicity in clinical practice we have investigated the EpoB toxic effect in vitro and we have characterized in vivo his general and neurological side effects in the Wistar and Fischer rats. The in vitro experiment performed in Dorsal Root Ganglia explants showed a dose-dependent effect of EpoB exposure on neurite elongation; concentrations equal to 50nM or higher induced a significant reduction in neurite elongation after 24h and this effect was even more severe after 48h. A dose-dependent neurotoxic effect was confirmed in both in vivo studies. In these models EpoB peripheral neurotoxicity was investigated with neurophysiological, behavioral (Hot plate test) and pathological (morphologic and morphometric analysis, Intraepidermal Nerve Fibers density) methods. Moreover, in order to evidence the EpoB effect at the molecular level we focused on tubulin and myelin proteins. All the results consistently demonstrated that EpoB was more toxic in Fischer than in Wistar rats at the general and neurological levels in the dose range 0,25-1,5 mg/kg. Our results describing the dose-dependent neurological effects of EpoB and demonstrating that tubulin hyper-polimerization occurs at neurotoxic doses can be a solid basis for future studies

Chiorazzi, A., Meregalli, C., Lombardi, R., Lauria, G., Roglio, I., Melcangi, R., et al. (2009). Epothilone B-induced toxic effects on peripheral nervous system: in vitro and in vivo experimental models. In JOURNAL OF THE PERIPHERAL NERVOUS SYSTEM (pp.8-8).

Epothilone B-induced toxic effects on peripheral nervous system: in vitro and in vivo experimental models

CHIORAZZI, ALESSIA
Primo
;
MEREGALLI, CRISTINA
Secondo
;
CAVALETTI, GUIDO ANGELO
Ultimo
2009

Abstract

Epothilones are a novel class of microtubule-targeting anticancer agents that have a similar mechanism of action to the taxanes (i.e. polymerization of tubulin dimers into microtubules and stabilization of preformed microtubules) but show antiproliferative activity in taxane-resistant tumor cells. In order to study the epothilone B (EpoB)-induced neurotoxicity in clinical practice we have investigated the EpoB toxic effect in vitro and we have characterized in vivo his general and neurological side effects in the Wistar and Fischer rats. The in vitro experiment performed in Dorsal Root Ganglia explants showed a dose-dependent effect of EpoB exposure on neurite elongation; concentrations equal to 50nM or higher induced a significant reduction in neurite elongation after 24h and this effect was even more severe after 48h. A dose-dependent neurotoxic effect was confirmed in both in vivo studies. In these models EpoB peripheral neurotoxicity was investigated with neurophysiological, behavioral (Hot plate test) and pathological (morphologic and morphometric analysis, Intraepidermal Nerve Fibers density) methods. Moreover, in order to evidence the EpoB effect at the molecular level we focused on tubulin and myelin proteins. All the results consistently demonstrated that EpoB was more toxic in Fischer than in Wistar rats at the general and neurological levels in the dose range 0,25-1,5 mg/kg. Our results describing the dose-dependent neurological effects of EpoB and demonstrating that tubulin hyper-polimerization occurs at neurotoxic doses can be a solid basis for future studies
paper
Epothilone B, Peripheral toxicity, Animal model
English
Meeting of the Italian-Peripheral-Nerve-Study-Group MAY 14-16
2009
JOURNAL OF THE PERIPHERAL NERVOUS SYSTEM
2009
14
8
8
open
Chiorazzi, A., Meregalli, C., Lombardi, R., Lauria, G., Roglio, I., Melcangi, R., et al. (2009). Epothilone B-induced toxic effects on peripheral nervous system: in vitro and in vivo experimental models. In JOURNAL OF THE PERIPHERAL NERVOUS SYSTEM (pp.8-8).
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Utilizza questo identificativo per citare o creare un link a questo documento: https://hdl.handle.net/10281/59198
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