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Comparative Plasma Exposure and Lung Distribution of Two Human Use Commercial Azithromycin Formulations Assessed in Murine Model: A Preclinical Study

Azithromycin (AZM) therapeutic failure and relapses of patients treated with generic formulations have been observed in clinical practice. The main goal of this research was to compare in a preclinical study the serum exposure and lung tissue concentration of two commercial formulations AZM-based in...

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Autores principales: Rivulgo, Virginia, Sparo, Mónica, Ceci, Mónica, Fumuso, Elida, Confalonieri, Alejandra, Delpech, Gastón, Sánchez Bruni, Sergio F.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Hindawi Publishing Corporation 2013
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3773390/
https://www.ncbi.nlm.nih.gov/pubmed/24073402
http://dx.doi.org/10.1155/2013/392010
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author Rivulgo, Virginia
Sparo, Mónica
Ceci, Mónica
Fumuso, Elida
Confalonieri, Alejandra
Delpech, Gastón
Sánchez Bruni, Sergio F.
author_facet Rivulgo, Virginia
Sparo, Mónica
Ceci, Mónica
Fumuso, Elida
Confalonieri, Alejandra
Delpech, Gastón
Sánchez Bruni, Sergio F.
author_sort Rivulgo, Virginia
collection PubMed
description Azithromycin (AZM) therapeutic failure and relapses of patients treated with generic formulations have been observed in clinical practice. The main goal of this research was to compare in a preclinical study the serum exposure and lung tissue concentration of two commercial formulations AZM-based in murine model. The current study involved 264 healthy Balb-C. Mice were divided into two groups (n = 44): animals of Group A (reference formulation -R-) were orally treated with AZM suspension at 10 mg/kg of b.w. Experimental animals of Group B (generic formulation -G-) received identical treatment than Group A with a generic formulation AZM-based. The study was repeated twice as Phase II and III. Serum and lung tissue samples were taken 24 h post treatment. Validated microbiological assay was used to determine the serum pharmacokinetic and lung distribution of AZM. After the pharmacokinetic analysis was observed, a similar serum exposure for both formulations of AZM assayed. In contrast, statistical differences (P < 0.001) were obtained after comparing the concentrations of both formulations in lung tissue, being the values obtained for AUC and Cmax (AZM-R-) +1586 and 122%, respectively, than those obtained for AZM-G- in lung. These differences may indicate large differences on the distribution process of both formulations, which may explain the lack of efficacy/therapeutic failure observed on clinical practice.
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spelling pubmed-37733902013-09-26 Comparative Plasma Exposure and Lung Distribution of Two Human Use Commercial Azithromycin Formulations Assessed in Murine Model: A Preclinical Study Rivulgo, Virginia Sparo, Mónica Ceci, Mónica Fumuso, Elida Confalonieri, Alejandra Delpech, Gastón Sánchez Bruni, Sergio F. Biomed Res Int Research Article Azithromycin (AZM) therapeutic failure and relapses of patients treated with generic formulations have been observed in clinical practice. The main goal of this research was to compare in a preclinical study the serum exposure and lung tissue concentration of two commercial formulations AZM-based in murine model. The current study involved 264 healthy Balb-C. Mice were divided into two groups (n = 44): animals of Group A (reference formulation -R-) were orally treated with AZM suspension at 10 mg/kg of b.w. Experimental animals of Group B (generic formulation -G-) received identical treatment than Group A with a generic formulation AZM-based. The study was repeated twice as Phase II and III. Serum and lung tissue samples were taken 24 h post treatment. Validated microbiological assay was used to determine the serum pharmacokinetic and lung distribution of AZM. After the pharmacokinetic analysis was observed, a similar serum exposure for both formulations of AZM assayed. In contrast, statistical differences (P < 0.001) were obtained after comparing the concentrations of both formulations in lung tissue, being the values obtained for AUC and Cmax (AZM-R-) +1586 and 122%, respectively, than those obtained for AZM-G- in lung. These differences may indicate large differences on the distribution process of both formulations, which may explain the lack of efficacy/therapeutic failure observed on clinical practice. Hindawi Publishing Corporation 2013 2013-08-29 /pmc/articles/PMC3773390/ /pubmed/24073402 http://dx.doi.org/10.1155/2013/392010 Text en Copyright © 2013 Virginia Rivulgo et al. https://creativecommons.org/licenses/by/3.0/ This is an open access article distributed under the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original work is properly cited.
spellingShingle Research Article
Rivulgo, Virginia
Sparo, Mónica
Ceci, Mónica
Fumuso, Elida
Confalonieri, Alejandra
Delpech, Gastón
Sánchez Bruni, Sergio F.
Comparative Plasma Exposure and Lung Distribution of Two Human Use Commercial Azithromycin Formulations Assessed in Murine Model: A Preclinical Study
title Comparative Plasma Exposure and Lung Distribution of Two Human Use Commercial Azithromycin Formulations Assessed in Murine Model: A Preclinical Study
title_full Comparative Plasma Exposure and Lung Distribution of Two Human Use Commercial Azithromycin Formulations Assessed in Murine Model: A Preclinical Study
title_fullStr Comparative Plasma Exposure and Lung Distribution of Two Human Use Commercial Azithromycin Formulations Assessed in Murine Model: A Preclinical Study
title_full_unstemmed Comparative Plasma Exposure and Lung Distribution of Two Human Use Commercial Azithromycin Formulations Assessed in Murine Model: A Preclinical Study
title_short Comparative Plasma Exposure and Lung Distribution of Two Human Use Commercial Azithromycin Formulations Assessed in Murine Model: A Preclinical Study
title_sort comparative plasma exposure and lung distribution of two human use commercial azithromycin formulations assessed in murine model: a preclinical study
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3773390/
https://www.ncbi.nlm.nih.gov/pubmed/24073402
http://dx.doi.org/10.1155/2013/392010
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