Efficacy of hepatitis B virus ribonuclease H inhibitors, a new class of replication antagonists, in FRG human liver chimeric mice.

Long, Kelly R; Lomonosova, Elena; Li, Qilan; Ponzar, Nathan L; Villa, Juan A; Touchette, Erin; Rapp, Stephen; Liley, R Matt; Murelli, Ryan P; Grigoryan, Alexandre; Buller, R Mark; Wilson, Lisa; Bial, John; Sagartz, John E; Tavis, John E

Long, Kelly R; Lomonosova, Elena; Li, Qilan; Ponzar, Nathan L; Villa, Juan A; Touchette, Erin; Rapp, Stephen; Liley, R Matt; Murelli, Ryan P; Grigoryan, Alexandre; Buller, R Mark; Wilson, Lisa; Bial, John; Sagartz, John E; Tavis, John E.

Affiliation

Long KR; Seventh Wave Laboratories LLC, 19 Worthington Access Drive, Maryland Heights, MO 63043, USA. Electronic address: klong@7thwavelabs.com.
Lomonosova E; Department of Molecular Microbiology and Immunology & the Saint Louis University Liver Center, Saint Louis University School of Medicine, 1100 S. Grand Blvd., St. Louis, MO 63104, USA. Electronic address: elena.lomonosova@health.slu.edu.
Li Q; Department of Molecular Microbiology and Immunology & the Saint Louis University Liver Center, Saint Louis University School of Medicine, 1100 S. Grand Blvd., St. Louis, MO 63104, USA. Electronic address: qilan.li@health.slu.edu.
Ponzar NL; Department of Molecular Microbiology and Immunology & the Saint Louis University Liver Center, Saint Louis University School of Medicine, 1100 S. Grand Blvd., St. Louis, MO 63104, USA. Electronic address: nathan.ponzar@slu.edu.
Villa JA; Department of Molecular Microbiology and Immunology & the Saint Louis University Liver Center, Saint Louis University School of Medicine, 1100 S. Grand Blvd., St. Louis, MO 63104, USA. Electronic address: juan.villatorrecilla@health.slu.edu.
Touchette E; Seventh Wave Laboratories LLC, 19 Worthington Access Drive, Maryland Heights, MO 63043, USA. Electronic address: etouchette@7thwavelabs.com.
Rapp S; Seventh Wave Laboratories LLC, 19 Worthington Access Drive, Maryland Heights, MO 63043, USA. Electronic address: srapp@7thwavelabs.com.
Liley RM; Seventh Wave Laboratories LLC, 19 Worthington Access Drive, Maryland Heights, MO 63043, USA. Electronic address: mliley@7thwavelabs.com.
Murelli RP; Brookyln College & PhD Program in Chemistry at the Graduate Center of the City University of New York, NY 11210, USA. Electronic address: rpmurelli@brooklyn.cuny.edu.
Grigoryan A; Brookyln College & PhD Program in Chemistry at the Graduate Center of the City University of New York, NY 11210, USA. Electronic address: alexgrigoryan@gmail.com.
Buller RM; Department of Molecular Microbiology and Immunology & the Saint Louis University Liver Center, Saint Louis University School of Medicine, 1100 S. Grand Blvd., St. Louis, MO 63104, USA.
Wilson L; Yecuris Corporation, P.O. Box 4645, Tualatin, OR 97062, USA. Electronic address: lisawilson@yecuris.com.
Bial J; Yecuris Corporation, P.O. Box 4645, Tualatin, OR 97062, USA. Electronic address: johnbial@yecuris.com.
Sagartz JE; Seventh Wave Laboratories LLC, 19 Worthington Access Drive, Maryland Heights, MO 63043, USA. Electronic address: jsagartz@7thwavelabs.com.
Tavis JE; Department of Molecular Microbiology and Immunology & the Saint Louis University Liver Center, Saint Louis University School of Medicine, 1100 S. Grand Blvd., St. Louis, MO 63104, USA. Electronic address: john.tavis@health.slu.edu.

Antiviral Res ; 149: 41-47, 2018 01.

Article in En | MEDLINE | ID: mdl-29129708

ABSTRACT

ABSTRACT

Chronic hepatitis B virus infection cannot be cured by current therapies, so new treatments are urgently needed. We recently identified novel inhibitors of the hepatitis B virus ribonuclease H that suppress viral replication in cell culture. Here, we employed immunodeficient FRG KO mice whose livers had been engrafted with primary human hepatocytes to ask whether ribonuclease H inhibitors can suppress hepatitis B virus replication in vivo. Humanized FRG KO mice infected with hepatitis B virus were treated for two weeks with the ribonuclease H inhibitors #110, an α-hydroxytropolone, and #208, an N-hydroxypyridinedione. Hepatitis B virus viral titers and S and e antigen plasma levels were measured. Treatment with #110 and #208 caused significant reductions in plasma viremia without affecting hepatitis B virus S or e antigen levels, and viral titers rebounded following treatment cessation. This is the expected pattern for inhibitors of viral DNA synthesis. Compound #208 suppressed viral titers of both hepatitis B virus genotype A and C isolates. These data indicate that Hepatitis B virus replication can be suppressed during infection in an animal by inhibiting the viral ribonuclease H, validating the ribonuclease H as a novel target for antiviral drug development.

Subject(s)

Antiviral Agents/pharmacology; Hepatitis B virus/drug effects; Hepatitis B virus/physiology; Ribonuclease H/antagonists & inhibitors; Virus Replication/drug effects; Animals; Antiviral Agents/administration & dosage; Antiviral Agents/pharmacokinetics; DNA Replication/drug effects; Genotype; Hepatitis B/drug therapy; Hepatitis B/virology; Humans; Mice; Mice, Knockout; Mice, Transgenic; Pilot Projects; Treatment Outcome

Key words

Antivirals; Chimeric mice; FRG; HBV; RNaseH

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Full text: 1 Collection: 01-internacional Database: MEDLINE Main subject: Antiviral Agents / Virus Replication / Hepatitis B virus / Ribonuclease H Limits: Animals / Humans Language: En Journal: Antiviral Res Year: 2018 Document type: Article

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