| Literature DB >> 27184067 |
Linda Männ1, Nora Kochupurakkal2, Christian Martin3, Eva Verjans4, Anika Klingberg1, Simon Sody5, Andreas Kraus1, Jill Dalimot1, Eileen Bergmüller1, Steffen Jung6, Sylvia Voortman7, Elke Winterhager7, Sven Brandau5, Natalio Garbi8, Michael Kurrer9, Urs Eriksson10,11, Matthias Gunzer1, Mike Hasenberg1.
Abstract
To assess the role of alveolar macrophages (AMs) during a pulmonary Aspergillus fumigatus infection AMs were depleted by intratracheal application of diphtheria toxin (DTX) to transgenic CD11c.DTR mice prior to fungal infection. Unexpectedly, all CD11c.DTR mice treated with DTX died within 4-5 days, whether being infected with A. fumigatus or not. Despite measurable impact of DTX on lung functional parameters, these constrictions could not explain the high mortality rate. Instead, DTX-treated CD11c.DTR animals developed fulminant myocarditis (FM) characterized by massive leukocyte infiltration and myocardial cell destruction, including central parts of the heart's stimulus transmission system. In fact, standard limb lead ECG recordings of diseased but not healthy mice showed a "Brugada"-like pattern with an abnormally high ST segment pointing to enhanced susceptibility for potential lethal arrhythmias. While CD11c.DTR mice are extensively used for the characterization of CD11c(+) cells, including dendritic cells, several studies have already mentioned adverse side effects following DTX treatment. Our results demonstrate that this limitation is based on severe myocarditis but not on the expected lung constrictions, and has to be taken into consideration if this animal model is used. Based on these properties, however, the CD11c.DTR mouse might serve as useful animal model for FM.Entities:
Keywords: CD11c.DTR ⋅ Conditional knockout ⋅ Diphtheria toxin ⋅ Infection ⋅ Myocarditis ⋅ Transgenic mice
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Year: 2016 PMID: 27184067 DOI: 10.1002/eji.201546245
Source DB: PubMed Journal: Eur J Immunol ISSN: 0014-2980 Impact factor: 5.532