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Literature DB >> 30224531

Identification of Compounds Targeting Hepatitis B Virus Core Protein Dimerization through a Split Luciferase Complementation Assay.

Xia-Fei Wei^1,2, Chun-Yang Gan¹, Jing Cui¹, Ying-Ying Luo¹, Xue-Fei Cai¹, Yi Yuan¹, Jing Shen¹, Zhi-Ying Li¹, Wen-Lu Zhang¹, Quan-Xin Long¹, Yuan Hu¹, Juan Chen¹, Ni Tang¹, Haitao Guo³, Ai-Long Huang^4,2, Jie-Li Hu^4,2.

Abstract

The capsid of the hepatitis B virus is an attractive antiviral target for developing therapies against chronic hepatitis B infection. Currently available core protein allosteric modulators (CpAMs) mainly affect one of the two major types of protein-protein interactions involved in the process of capsid assembly, namely, the interaction between the core dimers. Compounds targeting the interaction between two core monomers have not been rigorously screened due to the lack of screening models. We report here a cell-based assay in which the formation of core dimers is indicated by split luciferase complementation (SLC). Making use of this model, 2 compounds, Arbidol (umifenovir) and 20-deoxyingenol, were identified from a library containing 672 compounds as core dimerization regulators. Arbidol and 20-deoxyingenol inhibit the hepatitis B virus (HBV) DNA replication in vitro by decreasing and increasing the formation of core dimer and capsid, respectively. Our results provided a proof of concept for the cell model to be used to screen new agents targeting the step of core dimer and capsid formation.

Entities: Chemical Disease Species

Keywords: 20-deoxyingenol; Arbidol; cell model; compound screen; core protein; dimer; hepatitis B virus; split luciferase

Mesh：

Substances：

Year: 2018 PMID： 30224531 PMCID： PMC6256781 DOI： 10.1128/AAC.01302-18

Source DB: PubMed Journal: Antimicrob Agents Chemother ISSN： 0066-4804 Impact factor: 5.191

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9. Hepatitis B Virus Capsid Assembly Modulators, but Not Nucleoside Analogs, Inhibit the Production of Extracellular Pregenomic RNA and Spliced RNA Variants.

Authors: Angela M Lam; Suping Ren; Christine Espiritu; Mollie Kelly; Vincent Lau; Lingjie Zheng; George D Hartman; Osvaldo A Flores; Klaus Klumpp
Journal: Antimicrob Agents Chemother Date: 2017-07-25 Impact factor: 5.191

Identification of Compounds Targeting Hepatitis B Virus Core Protein Dimerization through a Split Luciferase Complementation Assay.

1. The split luciferase complementation assay.

2. NanoLuc Complementation Reporter Optimized for Accurate Measurement of Protein Interactions in Cells.

Review 3. Hepatitis B virus infection.

4. Structure-based design and biochemical evaluation of sulfanilamide derivatives as hepatitis B virus capsid assembly inhibitors.

5. Mapping of homologous interaction sites in the hepatitis B virus core protein.

6. Hepatitis core antigen produced in Escherichia coli: subunit composition, conformational analysis, and in vitro capsid assembly.

7. Benefits and risks of interferon therapy for hepatitis B.

8. An in vitro fluorescence screen to identify antivirals that disrupt hepatitis B virus capsid assembly.

9. Hepatitis B Virus Capsid Assembly Modulators, but Not Nucleoside Analogs, Inhibit the Production of Extracellular Pregenomic RNA and Spliced RNA Variants.

Review 10. Arbidol as a broad-spectrum antiviral: an update.

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Review 2. COVID-19 Antiviral and Treatment Candidates: Current Status.

3. Experimental and Analytical Framework for "Mix-and-Read" Assays Based on Split Luciferase.

Review 4. Efficacy and safety of arbidol (umifenovir) in patients with COVID-19: A systematic review and meta-analysis.