Tumor Necrosis Factor-α Receptor 1 Mediates Borna Disease Virus 1-Induced Changes in Peroxisomal and Mitochondrial Dynamics in Neurons

Borna disease virus 1 (BoDV1) causes a persistent infection in the mammalian brain. Peroxisomes and mitochondria play essential roles in the cellular antiviral immune response, but the effect of BoDV1 infection on peroxisomal and mitochondrial dynamics and their respective antioxidant capacities is...

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Veröffentlicht in:	International journal of molecular sciences 2024-02, Vol.25 (3), p.1849
Hauptverfasser:	Osei, Dominic, Baumgart-Vogt, Eveline, Ahlemeyer, Barbara, Herden, Christiane
Format:	Artikel
Sprache:	eng
Schlagworte:	Antioxidants Biosynthesis Brain Cytokines Encephalitis Enzymes Fatty acids Genetic engineering Immune response Immune system Infection Infections Inflammation Kinases Mitochondria Necrosis Neurons Polyamines Proteins Superoxide Tumor necrosis factor Tumor necrosis factor-TNF Tumors
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description	Borna disease virus 1 (BoDV1) causes a persistent infection in the mammalian brain. Peroxisomes and mitochondria play essential roles in the cellular antiviral immune response, but the effect of BoDV1 infection on peroxisomal and mitochondrial dynamics and their respective antioxidant capacities is still not clear. Using different mouse lines-i.e., tumor necrosis factor-α transgenic (TNFTg; to pro-inflammatory status), TNF receptor-1 knockout (TNFR1ko), and TNFR2ko mice in comparison to wild-type (Wt) mice-we analyzed the abundances of both organelles and their main antioxidant enzymes, catalase and superoxide dismutase 2 (SOD2), in neurons of the hippocampal, cerebral, and cerebellar cortices. In TNFTg mice, a strong increase in mitochondrial (6.9-fold) and SOD2 (12.1-fold) abundances was detected; meanwhile, peroxisomal abundance increased slightly (1.5-fold), but that of catalase decreased (2.9-fold). After BoDV1 infection, a strong decrease in mitochondrial (2.1-6.5-fold), SOD2 (2.7-9.1-fold), and catalase (2.7-10.3-fold) abundances, but a slight increase in peroxisomes (1.3-1.6-fold), were detected in Wt and TNFR2ko mice, whereas no changes occurred in TNFR1ko mice. Our data suggest that the TNF system plays a crucial role in the biogenesis of both subcellular organelles. Moreover, TNFR1 signaling mediated the changes in peroxisomal and mitochondrial dynamics after BoDV1 infection, highlighting new mechanisms by which BoDV1 may achieve immune evasion and viral persistence.
doi_str_mv	10.3390/ijms25031849
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subjects	Antioxidants Biosynthesis Brain Cytokines Encephalitis Enzymes Fatty acids Genetic engineering Immune response Immune system Infection Infections Inflammation Kinases Mitochondria Necrosis Neurons Polyamines Proteins Superoxide Tumor necrosis factor Tumor necrosis factor-TNF Tumors
title	Tumor Necrosis Factor-α Receptor 1 Mediates Borna Disease Virus 1-Induced Changes in Peroxisomal and Mitochondrial Dynamics in Neurons
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