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Antiviral Res
. 2021 Nov 23;105211.
doi: 10.1016/j.antiviral.2021.105211. Online ahead of print.
Preclinical characterization of AB-506, an inhibitor of HBV replication targeting the viral core protein
Nagraj Mani 1 , Andrew G Cole 2 , Janet R Phelps 2 , Andrzej Ardzinski 2 , Robbin Burns 2 , Tim Chiu 2 , Andrea Cuconati 2 , Bruce D Dorsey 2 , Ellen Evangelista 2 , Kristi Fan 2 , Fang Guo 2 , Troy O Harasym 2 , Salam Kadhim 2 , Roseann Kowalski 2 , Steven G Kultgen 2 , Amy C H Lee 2 , Alice H Li 2 , Sara A Majeski 2 , Angela Miller 2 , Chris Pasetka 2 , Stephen P Reid 2 , Rene Rijnbrand 2 , Holly M Micolochick Steuer 2 , Kim Stever 2 , Sunny Tang 2 , Xiaowei Teng 2 , Xiaohe Wang 2 , Michael J Sofia 2
Affiliations
Affiliations
1
Arbutus Biopharma Inc., 701 Veterans Circle, Warminster, PA, 18974, USA. Electronic address: [email protected].
2
Arbutus Biopharma Inc., 701 Veterans Circle, Warminster, PA, 18974, USA.
PMID: 34826506 DOI: 10.1016/j.antiviral.2021.105211
Abstract
AB-506, a small-molecule inhibitor targeting the HBV core protein, inhibits viral replication in vitro (HepAD38 cells: EC50 of 0.077 μM, CC50 > 25 μM) and in vivo (HBV mouse model: ∼3.0 log10 reductions in serum HBV DNA compared to the vehicle control). Binding of AB-506 to HBV core protein accelerates capsid assembly and inhibits HBV pgRNA encapsidation. Furthermore, AB-506 blocks cccDNA establishment in HBV-infected HepG2-hNTCP-C4 cells and primary human hepatocytes, leading to inhibition of viral RNA, HBsAg, and HBeAg production (EC50 from 0.64 μM to 1.92 μM). AB-506 demonstrated activity across HBV genotypes A-H and maintains antiviral activity against nucleos(t)ide analog-resistant variants in vitro. Evaluation of AB-506 against a panel of core variants showed that T33N/Q substitutions results in >200-fold increase in EC50 values, while L30F, L37Q, and I105T substitutions showed an 8 to 20-fold increase in EC50 values in comparison to the wild-type. In vitro combinations of AB-506 with NAs or an RNAi agent were additive to moderately synergistic. AB-506 exhibits good oral bioavailability, systemic exposure, and higher liver to plasma ratios in rodents, a pharmacokinetic profile supporting clinical development for chronic hepatitis B.
Keywords: AB-506; Aminoindane; CHB; Capsid inhibitor; HBV; pgRNA encapsidation.
Copyright © 2021. Published by Elsevier B.V.
Conflict of interest statement
Declaration of interests The authors declare the following financial interests/personal relationships which may be considered as potential competing interests: Authors include current or former employees of Arbutus Biopharma Inc., and may own company stock and/or patents.
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发表于 2021-11-28 04:14