Identification and analysis of hepatitis C virus NS3 helicase inhibitors using nucleic acid binding assays

Abstract: Typical assays used to discover and analyze small molecules that inhibit the hepatitis C virus (HCV) NS3 helicase yield few hits and are often confounded by compound interference. Oligonucleotide binding assays are examined here as an alternative. After comparing fluorescence polarization (FP), homogeneous time-resolved fluorescence (HTRF®; Cisbio) and AlphaScreen® (Perkin Elmer) assays, an FP-based assay was chosen to screen Sigma’s Library of Pharmacologically Active Compounds (LOPAC) for compounds that inhi… Show more

“…Among the resulting ligands, Suramin showed highest affinity for SFTSV-N. Suramin is a drug used for the treatment of trypanosomiasis and helminthiasis (37,38). Recently, its potential as an antineoplastic agent in the treatment of cancers and as an antiviral agent is being evaluated (39)(40)(41). Interestingly, while Suramin could bind SFTSV-N homologs such as RVFV-N (42), GRAV-N, and BUEV-N, it did not bind the Ns from other genera of the Bunyaviridae family (Orthobunyavirus, Nairovirus, and Hantavirus) or other viruses In the Suramin-bound structure of SFTSV-N, Suramin is found in the cavity encircling the central hole of the ring-like assembly.…”

Structure of Severe Fever with Thrombocytopenia Syndrome Virus Nucleocapsid Protein in Complex with Suramin Reveals Therapeutic Potential

“…Among the resulting ligands, Suramin showed highest affinity for SFTSV-N. Suramin is a drug used for the treatment of trypanosomiasis and helminthiasis (37,38). Recently, its potential as an antineoplastic agent in the treatment of cancers and as an antiviral agent is being evaluated (39)(40)(41). Interestingly, while Suramin could bind SFTSV-N homologs such as RVFV-N (42), GRAV-N, and BUEV-N, it did not bind the Ns from other genera of the Bunyaviridae family (Orthobunyavirus, Nairovirus, and Hantavirus) or other viruses In the Suramin-bound structure of SFTSV-N, Suramin is found in the cavity encircling the central hole of the ring-like assembly.…”

Structure of Severe Fever with Thrombocytopenia Syndrome Virus Nucleocapsid Protein in Complex with Suramin Reveals Therapeutic Potential

“…1A). All ATPase assays in this screen were performed in the absence of RNA (or DNA) because primuline derivatives are known to prevent NS3 from binding nucleic acids (10). RNA stimulates helicase-catalyzed ATP hydrolysis, and any compound that prevents RNA from binding NS3h would inhibit ATP hydrolysis in the presence of RNA.…”

“…Primuline is a fluorescent dye composed of a mixture of benzothiazole oligomers terminating with p-aminobenzene groups, and it prevents proteins from binding ssDNA or RNA (1,10). Li et al synthesized a series of chemical derivatives from a benzothiazole dimer purified from primuline, and they showed that some of these compounds potently and specifically inhibit HCV helicase (1).…”

“…Later, Mukherjee et al (10) showed that these primuline derivatives inhibit NS3h by displacing the protein after it is bound to its nucleic acid substrate. Unlike other compounds that simply compete with the DNA, the primuline derivatives, and related benzothiazole polymers like the dye titan yellow, cause NS3 to fall from DNA even in the absence of ATP (8,10), suggesting they can actively induce a protein conformational change needed to release the helicase protein from the nucleic acid tract on which it translocates (11,12).…”

Primuline Derivatives That Mimic RNA to Stimulate Hepatitis C Virus NS3 Helicase-catalyzed ATP Hydrolysis

“…Suramin has also been shown to block the binding or early steps of infection of several DNA and RNA viruses, like herpes simplex virus type-1 (Aguilar et al, 1999), cytomegalovirus (Baba et al, 1993), human hepatitis B virus (Schulze et al, 2007), hepatitis delta virus (Petcu et al, 1988), hepatitis C virus (Garson et al, 1999), dengue virus (Chen et al, 1997), several bunyaviruses (Crance et al, 1997;Ellenbecker et al, 2014;Iqbal et al, 2000;Jiao et al, 2013), norovirus-like particles (Tamura et al, 2004) and enterovirus 71 (Wang et al, 2014), for which the antiviral activity of suramin was also confirmed in an animal model (Ren et al, 2014). In recent in vitro studies suramin was identified as a hepatis C virus and dengue virus helicase inhibitor (Basavannacharya and Vasudevan, 2014;Mukherjee et al, 2012) and also as a norovirus RdRp inhibitor by virtual screening and biochemical assays with purified enzymes (Mastrangelo et al, 2012;Tarantino et al, 2014). In the present study we assessed the effect of suramin on CHIKV RNA synthesis using our recently established in vitro assay that relies on RTCs isolated from infected cells (Albulescu et al, 2014).…”

Suramin inhibits chikungunya virus replication through multiple mechanisms