<i>In Vitro</i>
            System for Modeling Influenza A Virus Resistance under Drug Pressure

Brown, Ashley N.; McSharry, James J.; Weng, Qingmei; Driebe, Elizabeth M.; Engelthaler, David M.; Sheff, Kelly; Keim, Paul; Nguyen, Jack; Drusano, George L.

doi:10.1128/aac.01385-09

Cited by 24 publications

(28 citation statements)

References 37 publications

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“…We used the hollow-fiber infection model (HIFM) system to study the response of the oseltamivir-resistant pandemic H1N1 influenza A virus, A/Hong Kong (H275Y), to zanamivir exposure. The use of the HFIM system for influenza A viruses has been described previously (6,22). Briefly, 10 2 MDCK cells infected with H1N1 A/Hong Kong influenza virus were mixed with 10 8 uninfected MDCK cells in 25 ml of VGM and were inoculated into the extracapillary space (ECS) of several hollow-fiber (HF) cartridges (FiberCell Systems, Frederick, MD).…”

Section: Virusesmentioning

confidence: 99%

“…Extracellular virus (V extra ) is the result of the egress of intracellular virus from the last intracellular virus compartment (V i5 ) and was assumed to be subject to a first-order loss rate constant (k loss,V extra ). The latter represents the degradation of virus in medium due to temperature sensitivity (6). The initial condition for extracellular virus was set to 0 PFU/ml, because the inoculum was free of intracellular virus.…”

Section: Virusesmentioning

confidence: 99%

“…(6), aliquoted, and stored at Ϫ80°C. MDCK cells (ATCC CCL-34) were obtained from the American Type Culture Collection (Manassas, VA) and were grown in minimal essential medium (MEM) supplemented with 10% fetal bovine serum (FBS), nonessential amino acids, 2 mM L-glutamine, 1 mM sodium pyruvate, 100 U/ml of penicillin, 100 g/ml of streptomycin, and 1.5 g/liter sodium bicarbonate at 37°C under 5% CO 2 .…”

mentioning

confidence: 99%

See 2 more Smart Citations

Effect of Half-Life on the Pharmacodynamic Index of Zanamivir against Influenza Virus Delineated by a Mathematical Model

Brown

Bulitta

McSharry

et al. 2011

Antimicrob Agents Chemother

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Section: Virusesmentioning

confidence: 99%

Section: Virusesmentioning

confidence: 99%

mentioning

confidence: 99%

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Effect of Half-Life on the Pharmacodynamic Index of Zanamivir against Influenza Virus Delineated by a Mathematical Model

Brown

Bulitta

McSharry

et al. 2011

Antimicrob Agents Chemother

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“…Influenza viruses have been shown to develop resistance to both NA inhibitors and adamantanes when serially passaged in the presence of the drugs in vitro (25,26). The drug-resistant viruses are viable, demonstrate decreased susceptibility to the drug in phenotypic assays, and possess mutations in the targeted protein (in the catalytic and/or framework residues of the NA protein after passage with NA inhibitors and in the transmembrane region of M2 protein after serial passage with adamantanes).…”

mentioning

confidence: 99%

T-705 (Favipiravir) Induces Lethal Mutagenesis in Influenza A H1N1 Viruses In Vitro

Baranovich

Wong

Armstrong

et al. 2013

J Virol

349

352

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Several novel anti-influenza compounds are in various phases of clinical development. One of these, T-705 (favipiravir), has a mechanism of action that is not fully understood but is suggested to target influenza virus RNA-dependent RNA polymerase. We investigated the mechanism of T-705 activity against influenza A (H1N1) viruses by applying selective drug pressure over multiple sequential passages in MDCK cells. We found that T-705 treatment did not select specific mutations in potential target proteins, including PB1, PB2, PA, and NP. Phenotypic assays based on cell viability confirmed that no T-705-resistant variants were selected. In the presence of T-705, titers of infectious virus decreased significantly (P < 0.0001) during serial passage in MDCK cells inoculated with seasonal influenza A (H1N1) viruses at a low multiplicity of infection (MOI; 0.0001 PFU/cell) or with 2009 pandemic H1N1 viruses at a high MOI (10 PFU/cell). There was no corresponding decrease in the number of viral RNA copies; therefore, specific virus infectivity (the ratio of infectious virus yield to viral RNA copy number) was reduced. Sequence analysis showed enrichment of G¡A and C¡T transversion mutations, increased mutation frequency, and a shift of the nucleotide profiles of individual NP gene clones under drug selection pressure. Our results demonstrate that T-705 induces a high rate of mutation that generates a nonviable viral phenotype and that lethal mutagenesis is a key antiviral mechanism of T-705. Our findings also explain the broad spectrum of activity of T-705 against viruses of multiple families.

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“…The HFIM system has been extensively described elsewhere (14)(15)(16). For these studies, H9 cells were infected with the IIIB strain of HIV-1 by incubating viral stocks with H9 cells for 1 week.…”

Section: Cells and Virusesmentioning

confidence: 99%

Pharmacokinetic Determinants of Virological Response to Raltegravir in the In Vitro Pharmacodynamic Hollow-Fiber Infection Model System

Brown

Adams

Baluya

et al. 2015

Antimicrob Agents Chemother

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Daily administration (q24h) of raltegravir has been shown to be as efficacious as twice-daily administration (q12h) in the hollow-fiber infection model (HFIM) system. However, q24h regimens were not noninferior to q12h dosing in a clinical trial. We hypothesized that between-patient variability in raltegravir pharmacokinetics (PK) was responsible for the discordance in conclusions between the in vitro and in vivo studies. Hollow-fiber cartridges were inoculated with HIV-infected H9 cells and uninfected CEM-SS cells. Four cartridges received the total daily exposure (800 mg) q24h and four received half the daily exposure (400 mg) q12h. PK profiles with half-lives of 8, 4, 3, and 2 h were simulated for each dosing interval. Cell-to-cell viral spread was assessed by flow cytometry. Viral inhibition was similar between q24h and q12h dosing at the 8-and 4-h half-lives. The q24h dosing was not as efficacious as the q12h dosing when faster half-lives were simulated; a lack of viral suppression was observed at days 3 and 4 for the 2-and 3-h half-lives, respectively. The discrepancy in conclusions between the in vitro HFIM system studies and clinical trials is likely due to the large interindividual variation in raltegravir PK. Raltegravir is an HIV-1 integrase inhibitor that is used in combination with other antiretroviral agents to treat patients with HIV-1 infections. Raltegravir-based combination chemotherapeutic regimens have been shown to be well tolerated and highly efficacious in both treatment-naive (1-5) and treatment-experienced (6-8) patient populations compared to other combination regimens. Raltegravir is currently administered as a 400-mg twicedaily (BID) dose. A once-daily (QD) raltegravir regimen would be preferable in a clinical setting, since the convenience of a QD regimen would likely improve patient adherence.Previous work done by others has shown that, once bound, raltegravir remains in the active site of the HIV-1 integrase protein for a long time, demonstrating dissociative half-lives ranging from 7.3 to 8.8 h (9, 10). The long occupancy time of raltegravir in the binding pocket of viral integrase suggests that once-daily dosing (800 mg QD) may be as efficacious as the current regimen of 400 mg BID. Moreover, data generated using an in vitro pharmacodynamic (PD) hollow-fiber infection model (HFIM) system supported this speculation (11). Given the strong in vitro support of once-daily dosing, Merck conducted a phase 3 noninferiority trial to compare the efficacy of raltegravir administered as 800 mg QD to the standard dosage regimen of 400 mg BID. The findings of this clinical study showed that both regimens yielded high response rates in vivo, but once-daily dosing did not achieve the Ϫ10% noninferiority margin and was deemed not noninferior to the twice-daily regimen (12). Our objectives for this study were to explain the discordance in conclusions between the in vitro experiments and human clinical studies for raltegravir and to identify the pharmacokinetic-pharmacodynamic (PK-PD) determinants ...

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In Vitro System for Modeling Influenza A Virus Resistance under Drug Pressure

Cited by 24 publications

References 37 publications

Effect of Half-Life on the Pharmacodynamic Index of Zanamivir against Influenza Virus Delineated by a Mathematical Model

Effect of Half-Life on the Pharmacodynamic Index of Zanamivir against Influenza Virus Delineated by a Mathematical Model

T-705 (Favipiravir) Induces Lethal Mutagenesis in Influenza A H1N1 Viruses In Vitro

Pharmacokinetic Determinants of Virological Response to Raltegravir in the In Vitro Pharmacodynamic Hollow-Fiber Infection Model System

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