Literature DB >> 23359228

Psammaplin A inhibits hepatitis C virus NS3 helicase.

Kazi Abdus Salam1, Atsushi Furuta, Naohiro Noda, Satoshi Tsuneda, Yuji Sekiguchi, Atsuya Yamashita, Kohji Moriishi, Masamichi Nakakoshi, Masayoshi Tsubuki, Hidenori Tani, Junichi Tanaka, Nobuyoshi Akimitsu.   

Abstract

Hepatitis C virus (HCV) is the causative agent of hepatitis C, a chronic infectious disease that can lead to development of hepatocellular carcinoma. The NS3 nucleoside triphosphatase (NTPase)/helicase has an essential role in HCV replication, and is therefore an attractive target for direct-acting antiviral strategies. In this study, we employed high-throughput screening using a photo-induced electron transfer (PET) system to identify an inhibitor of NS3 helicase from marine organism extracts. We successfully identified psammaplin A as a novel NS3 inhibitor. The dose-response relationship clearly demonstrates the inhibition of NS3 RNA helicase and ATPase activities by psammaplin A, with IC₅₀ values of 17 and 32 μM, respectively. Psammaplin A has no influence on the apparent Km value (0.4 mM) of NS3 ATPase activity, and acts as a non-competitive inhibitor. Additionally, it inhibits the binding of NS3 to single-stranded RNA in a dose-dependent manner. Furthermore, psammaplin A shows an inhibitory effect on viral replication, with EC₅₀ values of 6.1 and 6.3 μM in subgenomic replicon cells derived from genotypes 1b and 2a, respectively. We postulate that psammaplin A is a potential anti-viral agent through the inhibition of ATPase, RNA binding and helicase activities of NS3.

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Year:  2013        PMID: 23359228     DOI: 10.1007/s11418-013-0742-7

Source DB:  PubMed          Journal:  J Nat Med        ISSN: 1340-3443            Impact factor:   2.343


  36 in total

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3.  Three conformational snapshots of the hepatitis C virus NS3 helicase reveal a ratchet translocation mechanism.

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4.  Psammaplin A, a natural phenolic compound, has inhibitory effect on human topoisomerase II and is cytotoxic to cancer cells.

Authors:  D Kim; I S Lee; J H Jung; C O Lee; S U Choi
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6.  Comparison of HCV-associated gene expression and cell signaling pathways in cells with or without HCV replicon and in replicon-cured cells.

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Authors:  A Takamizawa; C Mori; I Fuke; S Manabe; S Murakami; J Fujita; E Onishi; T Andoh; I Yoshida; H Okayama
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8.  Psammaplin A, a marine natural product, inhibits aminopeptidase N and suppresses angiogenesis in vitro.

Authors:  Joong Sup Shim; Hyi-Seung Lee; Jongheon Shin; Ho Jeong Kwon
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10.  Cytotoxicity of psammaplin A from a two-sponge association may correlate with the inhibition of DNA replication.

Authors:  Yahong Jiang; Eun-Young Ahn; Seung Hee Ryu; Dong-Kyoo Kim; Jang-Su Park; Hyun Joo Yoon; Song You; Burm-Jong Lee; Dong Seok Lee; Jee H Jung
Journal:  BMC Cancer       Date:  2004-09-30       Impact factor: 4.430

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Journal:  Appl Microbiol Biotechnol       Date:  2014-02-23       Impact factor: 4.813

2.  Identification and biochemical characterization of halisulfate 3 and suvanine as novel inhibitors of hepatitis C virus NS3 helicase from a marine sponge.

Authors:  Atsushi Furuta; Kazi Abdus Salam; Idam Hermawan; Nobuyoshi Akimitsu; Junichi Tanaka; Hidenori Tani; Atsuya Yamashita; Kohji Moriishi; Masamichi Nakakoshi; Masayoshi Tsubuki; Poh Wee Peng; Youichi Suzuki; Naoki Yamamoto; Yuji Sekiguchi; Satoshi Tsuneda; Naohiro Noda
Journal:  Mar Drugs       Date:  2014-01-21       Impact factor: 5.118

Review 3.  Bioactive Compounds from Marine Sponges: Fundamentals and Applications.

Authors:  Disha Varijakzhan; Jiun-Yan Loh; Wai-Sum Yap; Khatijah Yusoff; Rabiha Seboussi; Swee-Hua Erin Lim; Kok-Song Lai; Chou-Min Chong
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Review 4.  RNA helicases required for viral propagation in humans.

Authors:  John C Marecki; Binyam Belachew; Jun Gao; Kevin D Raney
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Review 5.  Hepatitis C virus NS3 inhibitors: current and future perspectives.

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Review 6.  Marine-Derived Secondary Metabolites as Promising Epigenetic Bio-Compounds for Anticancer Therapy.

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  6 in total

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