Author: Lee, Hâ€R.; Cho, Y. Y.; Lee, G. Y.; You, Dâ€g.; Yoo, Y. D.; Kim, Y. J.
Title: A direct role for hepatitis B virus X protein in inducing mitochondrial membrane permeabilization Cord-id: afulhpin Document date: 2018_1_24
ID: afulhpin
Snippet: Hepatitis B virus X protein (HBx) acts as a multifunctional protein that regulates intracellular signalling pathways during HBV infection. It has mainly been studied in terms of its interaction with cellular proteins. Here, we show that HBx induces membrane permeabilization independently of the mitochondrial permeability transition pore complex. We generated mitochondrial outer membraneâ€mimic liposomes to observe the direct effects of HBx on membranes. We found that HBx induced membrane permea
Document: Hepatitis B virus X protein (HBx) acts as a multifunctional protein that regulates intracellular signalling pathways during HBV infection. It has mainly been studied in terms of its interaction with cellular proteins. Here, we show that HBx induces membrane permeabilization independently of the mitochondrial permeability transition pore complex. We generated mitochondrial outer membraneâ€mimic liposomes to observe the direct effects of HBx on membranes. We found that HBx induced membrane permeabilization, and the region comprising the transmembrane domain and the mitochondrialâ€targeting sequence was sufficient for this process. Membrane permeabilization was inhibited by nonselective channel blockers or by Nâ€(nâ€nonyl)deoxynojirimycin (NNâ€DNJ), a viroporin inhibitor. Moreover, NNâ€DNJ inhibited HBxâ€induced mitochondrial depolarization in Huhâ€7 cells. Based on the results of this study, we can postulate that the HBx protein itself is sufficient to induce mitochondrial membrane permeabilization. Our finding provides important information for a strategy of HBx targeting during HBV treatment.
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