A Novel Tricyclic Polyketide, Vanitaracin A, Specifically Inhibits the Entry of Hepatitis B and D Viruses by Targeting Sodium Taurocholate Cotransporting Polypeptide

Manabu Kaneko; Koichi Watashi; Shinji Kamisuki; Hiroki Matsunaga; Masashi Iwamoto; Fumihiro Kawai; Hirofumi Ohashi; Senko Tsukuda; Satomi Shimura; Ryosuke Suzuki; Hideki Aizaki; Masaya Sugiyama; Sam-Yong Park; Takayoshi Ito; Naoko Ohtani; Fumio Sugawara; Yasuhito Tanaka; Masashi Mizokami; Camille Sureau; Takaji Wakita

doi:10.1128/JVI.01855-15

A Novel Tricyclic Polyketide, Vanitaracin A, Specifically Inhibits the Entry of Hepatitis B and D Viruses by Targeting Sodium Taurocholate Cotransporting Polypeptide

J Virol. 2015 Dec;89(23):11945-53. doi: 10.1128/JVI.01855-15. Epub 2015 Sep 16.

Authors

Manabu Kaneko¹, Koichi Watashi², Shinji Kamisuki³, Hiroki Matsunaga³, Masashi Iwamoto¹, Fumihiro Kawai⁴, Hirofumi Ohashi¹, Senko Tsukuda⁵, Satomi Shimura⁶, Ryosuke Suzuki⁷, Hideki Aizaki⁷, Masaya Sugiyama⁸, Sam-Yong Park⁴, Takayoshi Ito⁹, Naoko Ohtani³, Fumio Sugawara³, Yasuhito Tanaka¹⁰, Masashi Mizokami⁸, Camille Sureau¹¹, Takaji Wakita⁷

Affiliations

¹ Department of Virology II, National Institute of Infectious Diseases, Tokyo, Japan Department of Applied Biological Science, Tokyo University of Science, Noda, Japan.
² Department of Virology II, National Institute of Infectious Diseases, Tokyo, Japan Department of Applied Biological Science, Tokyo University of Science, Noda, Japan kwatashi@nih.go.jp.
³ Department of Applied Biological Science, Tokyo University of Science, Noda, Japan.
⁴ Protein Design Laboratory, Yokohama City University, Yokohama, Japan.
⁵ Department of Virology II, National Institute of Infectious Diseases, Tokyo, Japan Micro-Signaling Regulation Technology Unit, RIKEN Center for Life Science Technologies, Wako, Japan.
⁶ Department of Virology II, National Institute of Infectious Diseases, Tokyo, Japan Scynexis, Inc., Durham, North Carolina, USA.
⁷ Department of Virology II, National Institute of Infectious Diseases, Tokyo, Japan.
⁸ Research Center for Hepatitis and Immunology, National Center for Global Health and Medicine, Ichikawa, Japan.
⁹ Digestive Diseases Center, Showa University Koto-Toyosu Hospital, Tokyo, Japan.
¹⁰ Department of Virology and Liver Unit, Nagoya City University Graduate School of Medicinal Sciences, Nagoya, Japan.
¹¹ Laboratoire de Virologie Moléculaire, Institut National de la Transfusion Sanguine, Paris, France.

Abstract

Anti-hepatitis B virus (HBV) drugs are currently limited to nucleos(t)ide analogs (NAs) and interferons. A challenge of drug development is the identification of small molecules that suppress HBV infection from new chemical sources. Here, from a fungus-derived secondary metabolite library, we identify a structurally novel tricyclic polyketide, named vanitaracin A, which specifically inhibits HBV infection. Vanitaracin A inhibited the viral entry process with a submicromolar 50% inhibitory concentration (IC50) (IC50 = 0.61 ± 0.23 μM), without evident cytotoxicity (50% cytotoxic concentration of >256 μM; selectivity index value of >419) in primary human hepatocytes. Vanitaracin A did not affect the HBV replication process. This compound was found to directly interact with the HBV entry receptor sodium taurocholate cotransporting polypeptide (NTCP) and impaired its bile acid transport activity. Consistent with this NTCP targeting, antiviral activity of vanitaracin A was observed with hepatitis D virus (HDV) but not hepatitis C virus. Importantly, vanitaracin A inhibited infection by all HBV genotypes tested (genotypes A to D) and clinically relevant NA-resistant HBV isolate. Thus, we identified a fungal metabolite, vanitaracin A, which was a potent, well-tolerated, and broadly active inhibitor of HBV and HDV entry. This compound, or its related analogs, could be part of an antiviral strategy for preventing reinfection with HBV, including clinically relevant nucleos(t)ide analog-resistant virus.

Importance: For achieving better treatment and prevention of hepatitis B virus (HBV) infection, anti-HBV agents targeting a new molecule are in great demand. Although sodium taurocholate cotransporting polypeptide (NTCP) has recently been reported to be an essential host factor for HBV entry, there is a limited number of reports that identify new compounds targeting NTCP and inhibiting HBV entry. Here, from an uncharacterized chemical library, we isolated a structurally new compound, named vanitaracin A, which inhibited the process of entry of HBV and hepatitis D virus (HDV). This compound was suggested to directly interact with NTCP and inhibit its transporter activity. Importantly, vanitaracin A inhibited the entry of all HBV genotypes examined and of a clinically relevant nucleos(t)ide analog-resistant HBV isolate.

Publication types

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

MeSH terms

Cell Line
DNA Primers / genetics
Drug Discovery / methods
Fluorescent Antibody Technique, Indirect
Hepatitis B / drug therapy*
Hepatitis B virus / physiology*
Hepatitis Delta Virus / physiology*
Humans
Luminescent Measurements
Organic Anion Transporters, Sodium-Dependent / metabolism*
Polyketides / pharmacology*
Real-Time Polymerase Chain Reaction
Reverse Transcriptase Polymerase Chain Reaction
Small Molecule Libraries
Surface Plasmon Resonance
Symporters / metabolism*
Talaromyces / chemistry*
Virus Internalization / drug effects*

Substances

DNA Primers
Organic Anion Transporters, Sodium-Dependent
Polyketides
Small Molecule Libraries
Symporters
vanitaracin A
sodium-bile acid cotransporter