Ebola viral dynamics in nonhuman primates provides insights into virus immuno-pathogenesis and antiviral strategies

Madelain, Vincent; Baize, Sylvain; Jacquot, Frédéric; Reynard, Stéphanie; Fizet, Alexandra; Barron, Stéphane; Solas, Caroline; Lacarelle, Bruno; Carbonnelle, Caroline; Raoul, Hervé; Lamballerie, Xavier de; Guedj, Jérémie

doi:10.1038/s41467-018-06215-z

Cited by 62 publications

(111 citation statements)

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“…We modeled the virologic and PK data that had been collected in the 44 animals of different experiments conducted in the BSL4 (see above), and complemented them with additional data on the innate and the adaptive immune responses 69 . A number of cytokines were measured longitudinally in a subset of macaques ( n = 20) using Luminex technology or enzyme‐linked immunosorbent assay, in particular IFNα, IL6, and TNFα, and cytometry measures were performed in the last experiment ( n = 10, 5 untreated and 5 treated with 180 mg/kg b.i.d.)…”

Section: Modeling Evd Progression In Nhps Treated With Favipiravir Usmentioning

confidence: 99%

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Modeling Favipiravir Antiviral Efficacy Against Emerging Viruses: From Animal Studies to Clinical Trials

Madelain

Mentré

Baize

et al. 2020

CPT Pharmacom & Syst Pharma

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on behalf of the Reaction! Research GroupIn 2014, our research network was involved in the evaluation of favipiravir, an anti-influenza polymerase inhibitor, against Ebola virus. In this review, we discuss how mathematical modeling was used, first to propose a relevant dosing regimen in humans, and then to optimize its antiviral efficacy in a nonhuman primate (NHP) model. The data collected in NHPs were finally used to develop a model of Ebola pathogenesis integrating the interactions among the virus, the innate and adaptive immune response, and the action of favipiravir. We conclude the review of this work by discussing how these results are of relevance for future human studies in the context of Ebola virus, but also for other emerging viral diseases for which no therapeutics are available.

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Section: Modeling Evd Progression In Nhps Treated With Favipiravir Usmentioning

confidence: 99%

“…Model predictions (median and 95% prediction interval) for the compartments of the integrated model given in Figure in animals left untreated (black) or treated with favipiravir 180 mg/kg BID 69 . The dots are the individual data in each compartment.…”

Section: Modeling Evd Progression In Nhps Treated With Favipiravir Usmentioning

confidence: 99%

Modeling Favipiravir Antiviral Efficacy Against Emerging Viruses: From Animal Studies to Clinical Trials

Madelain

Mentré

Baize

et al. 2020

CPT Pharmacom & Syst Pharma

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“…More complex models that account for EBOV viral titer kinetics, susceptible cells, EBOV-infected cells, and immune response dynamics might advance understanding of EVD pathogenesis and assist in prioritization of therapies for rigorous evaluation in randomized clinical trials (RCTs) [3]. Recently, Madelain et al [4] developed a single-anatomic compartment immuno-pathogenesis mathematical model to provide insights into EBOV-host dynamics in nonhuman primates and predict effectiveness of favipiravir and remdesivir, both viral RNA polymerase inhibitors, for post exposure prophylaxis and treatment of EVD in humans.…”

Section: Introductionmentioning

confidence: 99%

Modeling Challenges of Ebola Virus–Host Dynamics during Infection and Treatment

Chertow

Shekhtman

Lurie

et al. 2020

Viruses

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Mathematical modeling of Ebola virus (EBOV)–host dynamics during infection and treatment in vivo is in its infancy due to few studies with frequent viral kinetic data, lack of approved antiviral therapies, and limited insight into the timing of EBOV infection of cells and tissues throughout the body. Current in-host mathematical models simplify EBOV infection by assuming a single homogeneous compartment of infection. In particular, a recent modeling study assumed the liver as the largest solid organ targeted by EBOV infection and predicted that nearly all cells become refractory to infection within seven days of initial infection without antiviral treatment. We compared our observations of EBOV kinetics in multiple anatomic compartments and hepatocellular injury in a critically ill patient with Ebola virus disease (EVD) with this model’s predictions. We also explored the model’s predictions, with and without antiviral therapy, by recapitulating the model using published inputs and assumptions. Our findings highlight the challenges of modeling EBOV–host dynamics and therapeutic efficacy and emphasize the need for iterative interdisciplinary efforts to refine mathematical models that might advance understanding of EVD pathogenesis and treatment.

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“…Remdesivir (GS-5734) acts by RNA-dependent RNA polymerase (RdRp)-mediated mechanism and prevents its proliferation 3 , even in the setting of intact exoribonuclease (ExoN)-mediated proofreading in viruses. In non-human primates, early initiation of polymerase inhibitors Favipiravir and Remdesivir improves survival, but whether they could be effective in patients is unknown 4 . Vincent Madelain et al 4 predicts survival rates of 60% for Favipiravir and 100% for Remdesivir when treatment is initiated within 3 and 4 days post infection, respectively.…”

mentioning

confidence: 99%

“…In non-human primates, early initiation of polymerase inhibitors Favipiravir and Remdesivir improves survival, but whether they could be effective in patients is unknown 4 . Vincent Madelain et al 4 predicts survival rates of 60% for Favipiravir and 100% for Remdesivir when treatment is initiated within 3 and 4 days post infection, respectively. ZMapp is a combination of three humanized monoclonal antibodies, that was produced by the method of genetic modification of the most consumable tobacco plants,that target three Ebola virus major glycoprotein and its Epitopes.This monoclonal antibody drug has been shown survival benefit in experimental non-human primates that was infected with this Ebola virus 5 .…”

mentioning

confidence: 99%