The difficulty in mimicking nervous system complexity and cell-cell interactions as well as the lack of kinetics information has limited the use of in vitro neurotoxicity data. Here, we assessed the biokinetic profile as well as the neurotoxicity of Amiodarone after acute and repeated exposure in two advanced rodent brain cell culture models, consisting of both neurons and glial cells organized in 2 or 3 dimensions to mimic the brain histiotypic structure and function. A strategy was applied to evidence the abiotic processes possibly affecting Amiodarone in vitro bioavailability, showing its ability to adsorb to the plastic devices. At clinically relevant Amiodarone concentrations, known to induce neurotoxicity in some patients during therapeutic treatment, a complete uptake was observed in both models in 24h, after single exposure. After repeated treatments, bioaccumulation was observed, especially in the 3D cell model, together with a greater alteration of neurotoxicity markers. After 14 days, Amiodarone major oxidative metabolite (mono-Ndesethylamiodarone) was detected at limited levels, indicating the presence of active drug metabolism enzymes (i.e. cytochrome P450) in both models. The assessment of biokinetics provides useful information on the relevance of in vitro toxicity data and should be considered in the design of an Integrated Testing Strategy aimed to identify specific neurotoxic alerts, and to improve the neurotoxicity assay predictivity for human acute and repeated exposure.

Amiodarone biokinetics, the formation of its major metabolite and neurotoxicity after acute and repeated exposure of brain cell cultures / Pomponio, Giuliana; Marie Gabrielle, Zurich; Luise, Schultz; Dieter G., Weiss; Romanelli, Luca; Alexandra, Gramowski; Emma Di, Consiglio; Emanuela, Testai. - In: TOXICOLOGY IN VITRO. - ISSN 0887-2333. - STAMPA. - 30:1(2015), pp. 192-202. [doi:10.1016/j.tiv.2015.01.012]

Amiodarone biokinetics, the formation of its major metabolite and neurotoxicity after acute and repeated exposure of brain cell cultures

POMPONIO, GIULIANA;ROMANELLI, LUCA;
2015

Abstract

The difficulty in mimicking nervous system complexity and cell-cell interactions as well as the lack of kinetics information has limited the use of in vitro neurotoxicity data. Here, we assessed the biokinetic profile as well as the neurotoxicity of Amiodarone after acute and repeated exposure in two advanced rodent brain cell culture models, consisting of both neurons and glial cells organized in 2 or 3 dimensions to mimic the brain histiotypic structure and function. A strategy was applied to evidence the abiotic processes possibly affecting Amiodarone in vitro bioavailability, showing its ability to adsorb to the plastic devices. At clinically relevant Amiodarone concentrations, known to induce neurotoxicity in some patients during therapeutic treatment, a complete uptake was observed in both models in 24h, after single exposure. After repeated treatments, bioaccumulation was observed, especially in the 3D cell model, together with a greater alteration of neurotoxicity markers. After 14 days, Amiodarone major oxidative metabolite (mono-Ndesethylamiodarone) was detected at limited levels, indicating the presence of active drug metabolism enzymes (i.e. cytochrome P450) in both models. The assessment of biokinetics provides useful information on the relevance of in vitro toxicity data and should be considered in the design of an Integrated Testing Strategy aimed to identify specific neurotoxic alerts, and to improve the neurotoxicity assay predictivity for human acute and repeated exposure.
2015
amiodarone; biokinetics; brain cell cultures
01 Pubblicazione su rivista::01a Articolo in rivista
Amiodarone biokinetics, the formation of its major metabolite and neurotoxicity after acute and repeated exposure of brain cell cultures / Pomponio, Giuliana; Marie Gabrielle, Zurich; Luise, Schultz; Dieter G., Weiss; Romanelli, Luca; Alexandra, Gramowski; Emma Di, Consiglio; Emanuela, Testai. - In: TOXICOLOGY IN VITRO. - ISSN 0887-2333. - STAMPA. - 30:1(2015), pp. 192-202. [doi:10.1016/j.tiv.2015.01.012]
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Utilizza questo identificativo per citare o creare un link a questo documento: https://hdl.handle.net/11573/690865
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