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Human cytomegalovirus infection increases mitochondrial biogenesis |
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| Authors: | Kaarbø Mari Ager-Wick Eirill Osenbroch Pia Øistad Kilander Anette Skinnes Ragnhild Müller Fredrik Eide Lars |
| Institution: | aDepartment of Microbiology and Department of Medical Biochemistry, Institute of Clinical Medicine, University of Oslo, Oslo University Hospital and Centre of Molecular Biology and Neuroscience, Oslo, Norway |
| Abstract: | Fibroblasts infected by Human Cytomegalovirus (CMV) undergo a robust increase in mitochondrial biogenesis with a corresponding increase in mitochondrial activity that is partly dependent on the viral anti-apoptotic pUL37x1 protein (vMIA). The increased respiration activity is blocked by the mitochondrial translation inhibitor chloramphenicol, which additionally suppresses viral production. Intriguingly, chloramphenicol and pUL37x1 depletion have different effects on respiration capacity but similar effects on CMV production, suggesting that pUL37x1 promotes viral replication by efficient utilization of new mitochondria. These results argue for a role of pUL37x1 beyond controlling apoptosis. |
| Keywords: | Abbreviations: CMV Human Cytomegalovirus ROS reactive oxygen species cI&ndash V complex I&ndash V PGC-1α peroxisomal proliferator-activated receptor gamma coactivator 1α NAO nonyl acridine orange |
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