Discovery of a first-in-class orally available HBV cccDNA inhibitor

Li Wang; Qihui Zhu; Jitao David Zhang; Yaling Zhang; Xiaoju Ni; Kunlun Xiang; Jiaxi Jiang; Baocun Li; Youjun Yu; Hui Hu; Meifang Zhang; Waikwong Wu; Jing Zeng; Zhipeng Yan; Jieyu Dai; Kai Sun; Xin Zhang; Dongdong Chen; Song Feng; Lisa Sach-Peltason; John A T Young; Lu Gao

doi:10.1016/j.jhep.2022.12.014

Discovery of a first-in-class orally available HBV cccDNA inhibitor

J Hepatol. 2023 Apr;78(4):742-753. doi: 10.1016/j.jhep.2022.12.014. Epub 2022 Dec 30.

Authors

Li Wang¹, Qihui Zhu¹, Jitao David Zhang², Yaling Zhang¹, Xiaoju Ni¹, Kunlun Xiang¹, Jiaxi Jiang¹, Baocun Li¹, Youjun Yu¹, Hui Hu¹, Meifang Zhang³, Waikwong Wu³, Jing Zeng¹, Zhipeng Yan¹, Jieyu Dai², Kai Sun², Xin Zhang⁴, Dongdong Chen⁵, Song Feng⁵, Lisa Sach-Peltason⁶, John A T Young⁷, Lu Gao⁸

Affiliations

¹ Infectious Disease Discovery.
² Pharmaceutical Sciences.
³ Lead Discovery.
⁴ Preclinical Chemistry Manufacturing and Controls.
⁵ Medicinal Chemistry.
⁶ Data & Analytics, Roche Pharmaceutical Research and Early Development, Roche Innovation Center Shanghai, Roche Innovation Center Basel.
⁷ Infectious Disease Discovery. Electronic address: john.young.jy3@Roche.com.
⁸ Infectious Disease Discovery. Electronic address: goodlucksept2016@yahoo.com.

PMID: 36587899
DOI: 10.1016/j.jhep.2022.12.014

Abstract

Background & aims: The persistence of covalently closed circular DNA (cccDNA) in infected hepatocytes is the major barrier preventing viral eradication with existing therapies in patients with chronic hepatitis B. Therapeutic agents that can eliminate cccDNA are urgently needed to achieve viral eradication and thus HBV cure.

Methods: A phenotypic assay with HBV-infected primary human hepatocytes (PHHs) was employed to screen for novel cccDNA inhibitors. A HBVcircle mouse model and a uPA-SCID (urokinase-type plasminogen activator-severe combined immunodeficiency) humanized liver mouse model were used to evaluate the anti-HBV efficacy of the discovered cccDNA inhibitors.

Results: Potent and dose-dependent reductions in extracellular HBV DNA, HBsAg, and HBeAg levels were achieved upon the initiation of ccc_R08 treatment two days after the HBV infection of PHHs. More importantly, the level of cccDNA was specifically reduced by ccc_R08, while it did not obviously affect mitochondrial DNA. Additionally, ccc_R08 showed no significant cytotoxicity in PHHs or in multiple proliferating cell lines. The twice daily oral administration of ccc_R08 to HBVcircle model mice, which contained surrogate cccDNA molecules, significantly decreased the serum levels of HBV DNA and antigens, and these effects were sustained during the off-treatment follow-up period. Moreover, at the end of follow-up, the levels of surrogate cccDNA molecules in the livers of ccc_R08-treated HBVcircle mice were reduced to below the lower limit of quantification.

Conclusions: We have discovered a small-molecule cccDNA inhibitor that reduces HBV cccDNA levels. cccDNA inhibitors potentially represent a new approach to completely cure patients chronically infected with HBV.

Impact and implications: Covalently closed circular DNA (cccDNA) persistence in HBV-infected hepatocytes is the root cause of chronic hepatitis B. We discovered a novel small-molecule cccDNA inhibitor that can specifically reduce cccDNA levels in HBV-infected hepatocytes. This type of molecule could offer a new approach to completely cure patients chronically infected with HBV.

Keywords: HBV; cccDNA; inhibitor.

Publication types

Research Support, Non-U.S. Gov't

MeSH terms

Animals
Antiviral Agents / pharmacology
Antiviral Agents / therapeutic use
DNA, Circular / therapeutic use
DNA, Viral / genetics
Hepatitis B virus
Hepatitis B, Chronic* / drug therapy
Humans
Mice
Mice, SCID
Virus Replication

Substances

DNA, Circular
DNA, Viral
Antiviral Agents