| Literature DB >> 35434625 |
Andrew G Cole1, Steven G Kultgen1, Nagraj Mani1, Andrzej Ardzinski1, Kristi Yi Fan1, Emily P Thi1, Bruce D Dorsey1, Kim Stever1, Tim Chiu1, Sunny Tang1, Owen Daly1, Janet R Phelps1, Troy Harasym1, Andrea Olland2, Robert K Suto2, Michael J Sofia1.
Abstract
Disruption of the HBV viral life cycle with small molecules that prevent the encapsidation of pregenomic RNA and viral polymerase through binding to HBV core protein is a clinically validated approach to inhibiting HBV viral replication. Herein we report the further optimisation of clinical candidate AB-506 through core modification with a focus on increasing oral exposure and oral half-life. Maintenance of high levels of anti-HBV cellular potency in conjunction with improvements in pharmacokinetic properties led to multi-log10 reductions in serum HBV DNA following low, once-daily oral dosing for key analogues in a preclinical animal model of HBV replication. This journal is © The Royal Society of Chemistry.Entities:
Year: 2022 PMID: 35434625 PMCID: PMC8942244 DOI: 10.1039/d1md00318f
Source DB: PubMed Journal: RSC Med Chem ISSN: 2632-8682