| Literature DB >> 34162831 |
Michelle P Clark1,2, Thao Huynh3, Peter Revill3,4, Marc Pellegrini5,6, Gregor Ebert7,8,9, Shringar Rao10, Liana Mackiewicz1, Hugh Mason3, Shahla Romal10, Michael D Stutz1,2,11, Sang H Ahn12, Linda Earnest4, Vitina Sozzi3, Margaret Littlejohn3,13, Bang M Tran13, Norbert Wiedemann14, Elizabeth Vincan3,13,15, Joseph Torresi4, Hans J Netter3, Tokameh Mahmoudi10.
Abstract
A major unmet clinical need is a therapeutic capable of removing hepatitis B virus (HBV) genome from the liver of infected individuals to reduce their risk of developing liver cancer. A strategy to deliver such a therapy could utilize the ability to target and promote apoptosis of infected hepatocytes. Presently there is no clinically relevant strategy that has been shown to effectively remove persistent episomal covalently closed circular HBV DNA (cccDNA) from the nucleus of hepatocytes. We used linearized single genome length HBV DNA of various genotypes to establish a cccDNA-like reservoir in immunocompetent mice and showed that clinical-stage orally administered drugs that antagonize the function of cellular inhibitor of apoptosis proteins can eliminate HBV replication and episomal HBV genome in the liver. Primary human liver organoid models were used to confirm the clinical relevance of these results. This study underscores a clinically tenable strategy for the potential elimination of chronic HBV reservoirs in patients.Entities:
Year: 2021 PMID: 34162831 DOI: 10.1038/s41419-021-03924-0
Source DB: PubMed Journal: Cell Death Dis Impact factor: 8.469