Intratracheal administration of solutions in mice; development and validation of an optimized method with improved efficacy, reproducibility and accuracy
Publication date
2022-03-01
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Abstract
Animal models are still vital in the field of respiratory disease research. To improve the accuracy and consistency of the dose of specific compounds administered specifically in the respiratory tract, it is important to optimize and to compare the technique to currently available techniques. In this study, an optimized intubation-mediated intratracheal administration (IMIT) technique is described and compared to oropharyngeal aspiration (OA). Adult female Balb/c mice were treated with Evans Blue using IMIT or OA and sacrificed after a short recovery to observe the distribution of solutions throughout the lungs. Additionally, mice were treated with increasing doses of lipopolysaccharide (LPS) or saline to compare efficacy of both techniques. Inflammatory cell numbers in bronchoalveolar lavage were quantified 24 h post-administration. Evans Blue staining revealed a more homogeneous distribution and less variability among animals treated using IMIT as compared to OA. Higher inflammatory cell numbers were observed in IMIT mice compared to OA mice after exposure to vehicle or the lowest LPS concentration. This study shows that the optimized IMIT is superior to OA with regards to efficacy, reproducibility and accuracy. This IMIT method can be deployed to refine 3R animal welfare aspects of the experimental design and improve the reproducibility of respiratory disease mouse models.
Keywords
Instillation, Intratracheal, Intubation, Methods, Oropharyngeal, Toxicology, Pharmacology, SDG 3 - Good Health and Well-being
Citation
Pelgrim, C E, van Ark, I, Leusink-Muis, T, Brans, M A D, Braber, S, Garssen, J, van Helvoort, A, Kraneveld, A D & Folkerts, G 2022, 'Intratracheal administration of solutions in mice; development and validation of an optimized method with improved efficacy, reproducibility and accuracy', Journal of Pharmacological and Toxicological Methods, vol. 114, 107156, pp. 1-7. https://doi.org/10.1016/j.vascn.2022.107156