A Rapid Screening Assay Identifies Monotherapy with Interferon-ß and Combination Therapies with Nucleoside Analogs as Effective Inhibitors of Ebola Virus

McCarthy, Stephen D.S.; Majchrzak-Kita, Beata; Racine, Trina; Kozłowski, H; Baker, Darren P.; Hoenen, Thomas; Kobinger, Gary P.; Fish, Eleanor N.; Branch, Donald R.

doi:10.1371/journal.pntd.0004364

Cited by 54 publications

(45 citation statements)

References 32 publications

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“…A recent publication reported that HIV-1 drugs inhibit EBOV virus-like particles (trVLPs) that undergo a single cycle of transcription and replication [16]. The drugs showed activity alone or in combination against the transcription-competent trVLPs, but limited efficacy against EBOV-eGFP [16].…”

Section: Resultsmentioning

confidence: 99%

“…The drugs showed activity alone or in combination against the transcription-competent trVLPs, but limited efficacy against EBOV-eGFP [16]. To investigate further these findings, we repeated the studies using the same cell lines, compound source, time of drug addition, and length of infection time to compare with the conditions we used to perform the drug screen study on EBOV/Mak (S2 Fig).…”

Section: Resultsmentioning

confidence: 99%

“…We previously reported lamivudine had no antiviral activity against EBOV in Vero E6, Hep G2, or monocyte-derived macrophages (MDMs) infected with the 1995 EBOV Kikwit variant [15]. Given the continued interest of using lamivudine to treat EVD and the results of a recent article showing in vitro antiviral activity against EBOV infection [16], we further evaluated the efficacy of lamivudine and a second HIV-1 drug, zidovudine, in a broad range of infected cell lines. Tested cell lines included Vero E6, Huh 7, HeLa, Hep G2, and 293T cells, and primary MDMs, using varying multiplicities of infections (MOIs), drugs from different sources, and different time courses of drug treatment and assay endpoints.…”

Section: Introductionmentioning

confidence: 99%

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Evaluation of the Activity of Lamivudine and Zidovudine against Ebola Virus

Dyall

Hart

et al. 2016

PLoS ONE

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In the fall of 2014, an international news agency reported that patients suffering from Ebola virus disease (EVD) in Liberia were treated successfully with lamivudine, an antiviral drug used to treat human immunodeficiency virus-1 and hepatitis B virus infections. According to the report, 13 out of 15 patients treated with lamivudine survived and were declared free from Ebola virus disease. In this study, the anti-Ebola virus (EBOV) activity of lamivudine and another antiretroviral, zidovudine, were evaluated in a diverse set of cell lines against two variants of wild-type EBOV. Variable assay parameters were assessed to include different multiplicities of infection, lengths of inoculation times, and durations of dosing. At a multiplicity of infection of 1, lamivudine and zidovudine had no effect on EBOV propagation in Vero E6, Hep G2, or HeLa cells, or in primary human monocyte-derived macrophages. At a multiplicity of infection of 0.1, zidovudine demonstrated limited anti-EBOV activity in Huh 7 cells. Under certain conditions, lamivudine had low anti-EBOV activity at the maximum concentration tested (320 μM). However, lamivudine never achieved greater than 30% viral inhibition, and the activity was not consistently reproducible. Combination of lamivudine and zidovudine showed no synergistic antiviral activity. Independently, a set of in vitro experiments testing lamivudine and zidovudine for antiviral activity against an Ebola-enhanced green fluorescent protein reporter virus was performed at the Centers for Disease Control and Prevention. No antiviral activity was observed for either compound. A study evaluating the efficacy of lamivudine in a guinea pig model of EVD found no survival benefit. This lack of benefit was observed despite plasma lamivudine concentrations in guinea pig of about 4 μg/ml obtained in a separately conducted pharmacokinetics study. These studies found no evidence to support the therapeutic use of lamivudine for the treatment of EVD.

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Section: Resultsmentioning

confidence: 99%

Section: Resultsmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

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Evaluation of the Activity of Lamivudine and Zidovudine against Ebola Virus

Dyall

Hart

et al. 2016

PLoS ONE

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“…In this screen, the drug Tasigna was not retested due to compound unavailability, but additionally, the drug Gleevec was included since it was reported to operate via the same mechanism and demonstrated better in vitro efficacy. The in vitro screens used viral RNA levels as a readout based on previous antiviral testing work [33] and infectious doses of MOI 0.01–0.1, similar to levels used in other anti-EBOV testing studies [6,34,35]. Given that the compounds tested in our study were chosen due to their perceived potential effectiveness for use against EBOV, the negative results demonstrate the importance of testing therapies using the actual live pathogen to determine effects.…”

Section: Discussionmentioning

confidence: 99%

Antiviral Screening of Multiple Compounds against Ebola Virus

Dowall

Bewley

Watson

et al. 2016

Viruses

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In light of the recent outbreak of Ebola virus (EBOV) disease in West Africa, there have been renewed efforts to search for effective antiviral countermeasures. A range of compounds currently available with broad antimicrobial activity have been tested for activity against EBOV. Using live EBOV, eighteen candidate compounds were screened for antiviral activity in vitro. The compounds were selected on a rational basis because their mechanisms of action suggested that they had the potential to disrupt EBOV entry, replication or exit from cells or because they had displayed some antiviral activity against EBOV in previous tests. Nine compounds caused no reduction in viral replication despite cells remaining healthy, so they were excluded from further analysis (zidovudine; didanosine; stavudine; abacavir sulphate; entecavir; JB1a; Aimspro; celgosivir; and castanospermine). A second screen of the remaining compounds and the feasibility of appropriateness for in vivo testing removed six further compounds (ouabain; omeprazole; esomeprazole; Gleevec; D-LANA-14; and Tasigna). The three most promising compounds (17-DMAG; BGB324; and NCK-8) were further screened for in vivo activity in the guinea pig model of EBOV disease. Two of the compounds, BGB324 and NCK-8, showed some effect against lethal infection in vivo at the concentrations tested, which warrants further investigation. Further, these data add to the body of knowledge on the antiviral activities of multiple compounds against EBOV and indicate that the scientific community should invest more effort into the development of novel and specific antiviral compounds to treat Ebola virus disease.

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“…In another study, six doses of human IFN-β (10.5 ug/kg) administered subcutaneously (SC) extended the survival time of NHPs challenged with EBOV or Marburg virus , but did not improve the survival rate [53], suggesting that IFN treatments might be beneficial, but likely not fully protective by themselves. Based on the in vitro observation that IFN-β could inhibit the replication of recombinant EBOV in HEK293 cells more strongly than IFN-α could [55], a historically controlled clinical trial tested the efficacy of IFN-β-1a in nine EVD patients in Guinea [56]. Within 2 days following qRT-PCR-mediated confirmation of EVD, IFN-β-1a (30 ug/day) was administered SC to patients daily, until patients were tested negative for EBOV, or perished [56].…”

Section: Evd Immunotherapymentioning

confidence: 99%

Clinical Evaluation of Ebola Virus Disease Therapeutics

Liu

Wong

et al. 2017

Trends in Molecular Medicine

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Ebola virus disease (EVD) was first described over 40 years ago, but no treatment has been approved for humans. The 2013–2016 EVD outbreak in West Africa has expedited the clinical evaluation of several candidate therapeutics that act through different mechanisms, but with mixed results. Nevertheless, these studies are important because the accumulation of clinical data and valuable experience in conducting efficacy trials under emergency circumstances will lead to better implementation of similar studies in the future. Here, we summarize the results of EVD clinical trials, focus on the discussion of factors that may have potentially impeded the effectiveness of existing candidate therapeutics, and highlight considerations that may help meet the challenges ahead in the quest to develop clinically-approved drug(s).

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A Rapid Screening Assay Identifies Monotherapy with Interferon-ß and Combination Therapies with Nucleoside Analogs as Effective Inhibitors of Ebola Virus

Cited by 54 publications

References 32 publications

Evaluation of the Activity of Lamivudine and Zidovudine against Ebola Virus

Evaluation of the Activity of Lamivudine and Zidovudine against Ebola Virus

Antiviral Screening of Multiple Compounds against Ebola Virus

Clinical Evaluation of Ebola Virus Disease Therapeutics

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