作者
Nobuyo Higashi-Kuwata, Sanae Hayashi, Hiroki Kumamoto, Hiromi Ogata-Aoki, Debananda Das, David Venzon, Shin-ichiro Hattori, Haydar Bulut, Mai Hashimoto, Masaki Otagiri, Nobutoki Takamune, Naoki Kishimoto, David A Davis, Shogo Misumi, Masakazu Kakuni, Yasuhito Tanaka, Hiroaki Mitsuya
发表日期
2021/5/1
期刊
Journal of hepatology
卷号
74
期号
5
页码范围
1075-1086
出版商
Elsevier
简介
Background & Aims
While certain nucleos(t)ide reverse transcriptase inhibitors (NRTIs) are efficacious in treating HBV infection, their effects are yet to be optimized and the emergence of NRTI-resistant HBV variants is an issue because of the requirement for lifelong treatment. The development of agents that more profoundly suppress wild-type and drug-resistant HBVs, and that have a long-acting effect, are crucial to improve patient outcomes.
Methods
Herein, we synthesized a novel long-acting 4’-modified NRTI termed E-CFCP. We tested its anti-HBV activity in vitro, before evaluating its anti-HBV activity in HBV-infected human-liver-chimeric mice (PXB-mice). E-CFCP’s long-acting features and E-CFCP-triphosphate’s interactions with the HBV reverse transcriptase (HBV-RT) were examined.
Results
E-CFCP potently blocked HBVWTD1 production (IC50qPCR_cell=1.8 nM) in HepG2.2.15 cells and HBVWTC2 (IC50 …
学术搜索中的文章
N Higashi-Kuwata, S Hayashi, H Kumamoto… - Journal of hepatology, 2021