Literature DB >> 22644022

Identification of disubstituted sulfonamide compounds as specific inhibitors of hepatitis B virus covalently closed circular DNA formation.

Dawei Cai1, Courtney Mills, Wenquan Yu, Ran Yan, Carol E Aldrich, Jeffry R Saputelli, William S Mason, Xiaodong Xu, Ju-Tao Guo, Timothy M Block, Andrea Cuconati, Haitao Guo.   

Abstract

Hepatitis B virus (HBV) covalently closed circular DNA (cccDNA) plays a central role in viral infection and persistence and is the basis for viral rebound after the cessation of therapy, as well as the elusiveness of a cure even after extended treatment. Therefore, there is an urgent need for the development of novel therapeutic agents that directly target cccDNA formation and maintenance. By employing an innovative cell-based cccDNA assay in which secreted HBV e antigen is a cccDNA-dependent surrogate, we screened an in-house small-molecule library consisting of 85,000 drug-like compounds. Two structurally related disubstituted sulfonamides (DSS), termed CCC-0975 and CCC-0346, emerged and were confirmed as inhibitors of cccDNA production, with low micromolar 50% effective concentrations (EC(50)s) in cell culture. Further mechanistic studies demonstrated that DSS compound treatment neither directly inhibited HBV DNA replication in cell culture nor reduced viral polymerase activity in the in vitro endogenous polymerase assay but synchronously reduced the levels of HBV cccDNA and its putative precursor, deproteinized relaxed circular DNA (DP-rcDNA). However, DSS compounds did not promote the intracellular decay of HBV DP-rcDNA and cccDNA, suggesting that the compounds interfere primarily with rcDNA conversion into cccDNA. In addition, we demonstrated that CCC-0975 was able to reduce cccDNA biosynthesis in duck HBV-infected primary duck hepatocytes. This is the first attempt, to our knowledge, to identify small molecules that target cccDNA formation, and DSS compounds thus potentially serve as proof-of-concept drug candidates for development into therapeutics to eliminate cccDNA from chronic HBV infection.

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Year:  2012        PMID: 22644022      PMCID: PMC3421587          DOI: 10.1128/AAC.00473-12

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


  48 in total

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3.  Infection and uptake of duck hepatitis B virus by duck hepatocytes maintained in the presence of dimethyl sulfoxide.

Authors:  J C Pugh; J W Summers
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4.  Selective extraction of polyoma DNA from infected mouse cell cultures.

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5.  The insertion domain of the duck hepatitis B virus core protein plays a role in nucleocapsid assembly.

Authors:  Haitao Guo; Carol E Aldrich; Jeffry Saputelli; Chunxiao Xu; William S Mason
Journal:  Virology       Date:  2006-07-11       Impact factor: 3.616

6.  Evaluation of transcriptional efficiency of hepatitis B virus covalently closed circular DNA by reverse transcription-PCR combined with the restriction enzyme digestion method.

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7.  Hepatitis B: the virus and disease.

Authors:  T Jake Liang
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8.  Expansion and contraction of the hepatitis B virus transcriptional template in infected chimpanzees.

Authors:  Stefan F Wieland; Hans Christian Spangenberg; Robert Thimme; Robert H Purcell; Francis V Chisari
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  92 in total

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Journal:  Cold Spring Harb Perspect Med       Date:  2015-04-01       Impact factor: 6.915

Review 4.  Host functions used by hepatitis B virus to complete its life cycle: Implications for developing host-targeting agents to treat chronic hepatitis B.

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5.  T5 Exonuclease Hydrolysis of Hepatitis B Virus Replicative Intermediates Allows Reliable Quantification and Fast Drug Efficacy Testing of Covalently Closed Circular DNA by PCR.

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Review 6.  Toward Elimination of Hepatitis B Virus Using Novel Drugs, Approaches, and Combined Modalities.

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Journal:  Clin Liver Dis       Date:  2016-08-30       Impact factor: 6.126

7.  New horizon for radical cure of chronic hepatitis B virus infection.

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Review 8.  Treatment of hepatitis B virus: an update.

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Journal:  Future Microbiol       Date:  2016-11-18       Impact factor: 3.165

9.  Covalently closed-circular hepatitis B virus DNA reduction with entecavir or lamivudine.

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10.  Effects of amino acid substitutions in hepatitis B virus surface protein on virion secretion, antigenicity, HBsAg and viral DNA.

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Journal:  J Hepatol       Date:  2016-09-17       Impact factor: 25.083

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