Evaluation of Hepatotoxicity with Treatment Doses of Flucytosine and Amphotericin B for Invasive Fungal Infections

Author:

Folk Alexandra1,Cotoraci Coralia2,Balta Cornel3,Suciu Maria3,Herman Hildegard3,Boldura Oana Maria4,Dinescu Sorina5,Paiusan Lucian1,Ardelean Aurel3,Hermenean Anca36

Affiliation:

1. Department of Pathology, Faculty of Medicine, “Vasile Goldis” Western University of Arad, 86 Rebreanu Street, 310414 Arad, Romania

2. Department of Bioethics, Faculty of Medicine, “Vasile Goldis” Western University of Arad, 86 Rebreanu Street, 310414 Arad, Romania

3. Institute of Life Sciences, Vasile Goldis Western University of Arad, 86 Rebreanu, 310414 Arad, Romania

4. Faculty of Veterinary Medicine, Department of Chemistry, Biochemistry and Molecular Biology, Banat University of Agricultural Sciences and Veterinary Medicine “King Mihai I of Romania” Timisoara, 119 Calea Aradului, 300645 Timisoara, Romania

5. Department of Biochemistry and Molecular Biology, University of Bucharest, 91-95 Splaiul Independentei, 050095 Bucharest, Romania

6. Department of Histology, Faculty of Medicine, “Vasile Goldis” Western University of Arad, 86 Rebreanu Street, 310414 Arad, Romania

Abstract

Invasive fungal infection is a well-known cause of morbidity and mortality in immunocompromised patients. In this study we aimed to evaluate the hepatotoxicity induced by combined therapy of flucytosine and amphotericin B, at three different doses administered to mice for 14 days: 50 mg/kg flucytosine and 300 μg/kg amphotericin B; 100 mg/kg flucytosine and 600 μg/kg amphotericin B; 150 mg/kg flucytosine and 900 μg/kg amphotericin B. Liver injuries were evaluated by analysis of optic and electron microscopy samples, changes in TNF-α, IL-6, and NF-κB inflammation markers levels of expression, and evaluation of mRNA profiles. Histological and ultrastructural analysis revealed an increase in parenchymal and portal inflammation in mice and Kupffer cells activation. Combined antifungal treatment stimulated activation of an inflammatory pathway, demonstrated by a significant dose-dependent increase of TNF-αand IL-6 immunoreactivity, together with mRNA upregulation. Also, NF-κB was activated, as suggested by the high levels found in hepatic tissue and upregulation of target genes. Our results suggest that antifungal combined therapy exerts a synergistic inflammatory activation in a dose-dependent manner, through NF-κB pathway, which promotes an inflammatory cascade during inflammation. The use of combined antifungal therapy needs to be dose limiting due to the associated risk of liver injury, especially for those patients with hepatic dysfunction.

Funder

University of Bucharest

Publisher

Hindawi Limited

Subject

General Immunology and Microbiology,General Biochemistry, Genetics and Molecular Biology,General Medicine

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