Resistance of high fitness hepatitis C virus to lethal mutagenesis

Gallego, Isabel; Gregori, Josep; Soria, María Eugenia; García-Crespo, Carlos; García–Álvarez, Mónica; Gómez-González, Alfonso; Valiergue, Rosalie; Gómez, Jordi; Esteban, Juan Ignacio; Quer, Josep; Domingo, Esteban; Perales, Celia

doi:10.1016/j.virol.2018.07.030

Cited by 32 publications

(52 citation statements)

References 53 publications

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“…Here, we document inhibition of HCV replication by Gua in single and serial infections of Huh-7.5 cells that led to loss of infectivity without significant toxicity for the host cells. The antiviral action of Gua was also exerted on high fitness HCV, albeit without loss of infectivity after 5 passages in the presence of Gua, in agreement with the drug resistance phenotype displayed by high fitness HCV (Fig 1) [14][15][16][17]. The antiviral effect of Gua was not observed for FMDV in BHK-21 cells or for LCMV and VSV in Huh-7.5 cells (Fig 3).…”

Section: Discussionsupporting

confidence: 79%

“…The HCV p100 virus [HCV p0 passaged 100 times in Huh-7.5 reporter cells], shows a relative fitness that is 2.2 times higher than that of the HCV p0 parental population [14]. Since viral fitness can influence the response of the virus to antiviral agents [15][16][17], HCV p100 was used to study the response of a high fitness HCV to Gua. For this, HCV p100 was subjected to 5 serial passages in Huh-7.5 reporter cells using an initial m.o.i.…”

Section: Effect Of Gua On a High Fitness Hcv Populationmentioning

confidence: 99%

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Guanosine inhibits hepatitis C virus replication and increases indel frequencies, associated with altered intracellular nucleotide pools

Jareño

Ortega-Prieto

Díaz-Martínez

et al. 2020

Preprint

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In the course of experiments aimed at deciphering the inhibition mechanism of mycophenolic acid and ribavirin in hepatitis C virus (HCV) infection, we observed an inhibitory effect of the nucleoside guanosine (Gua). Here, we report that Gua and not the other standard nucleosides inhibits HCV replication in human hepatoma cells. Gua did not directly inhibit the in vitro polymerase activity of NS5B, but it modified the intracellular levels of nucleoside di-and triphosphate (NDPs and NTPs), leading to deficient HCV RNA replication and reduction of infectious progeny virus production. Changes in the concentrations of NTP or NDP modified NS5B RNA polymerase activity in vitro, in particular de novo RNA synthesis and template switching. Furthermore, the Gua-mediated changes were associated with a significant increase in the number of indels in viral RNA, which may account for the reduction of the specific infectivity of the viral progeny, suggesting the presence of defective genomes. Thus, a proper NTP:NDP balance appears to be critical to ensure HCV polymerase fidelity and minimal production of defective genomes. 3 32 33 34 35 36 37 38 39 40 41 42 43 44 45 46 Author summaryRibonucleoside metabolism is essential for replication of RNA viruses. In this article we describe the antiviral activity of the natural ribonucleoside guanosine (Gua). We demonstrate that hepatitis C virus (HCV) replication is inhibited in the presence of increasing concentrations of this ribonucleoside and that this inhibition does not occur as a consequence of a direct inhibition of HCV polymerase. Cells exposed to increasing concentrations of Gua show imbalances in the intracellular concentrations of nucleoside-diphosphates and triphosphates and as the virus is passaged in these cells, it accumulates mutations that reduce its infectivity and decimate its normal spreading capacity.imbalance of the concentrations of NDP and NTP results in the inhibition of HCV polymerase activity in vitro, and iv) Gua treatment is associated with an increase of indel frequency in progeny HCV RNA. The results provide evidence of a metabolism-dependent mechanism of generation of defective HCV genomes.including viral entry, primary translation and genome replication, overall efficiency of which is proportional to reporter gene activity [12]. The results (Fig 2A) show that a selective HCV entry inhibitor, hydroxyzine, strongly interferes with reporter gene accumulation, as previously documented [13] (Figure 2A). Of the four natural nucleosides, only Gua exerted a significant inhibitory role, as shown by reduced luciferase levels in these cells (Figure 2A), and suggesting that an early step of the infection preceding viral assembly is significantly inhibited by Gua. To further dissect the impact of Gua on HCV replication, we analyzed the effect of Gua, Ade, Cyt and Uri treatment at different times in the replication of a dicistronic subgenomic genotype 2a (JFH-1) replicon bearing a luciferase reporter gene [12]. The objective was to analyze if the effect took place at t...

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Section: Discussionsupporting

confidence: 79%

Section: Effect Of Gua On a High Fitness Hcv Populationmentioning

confidence: 99%

Guanosine inhibits hepatitis C virus replication and increases indel frequencies, associated with altered intracellular nucleotide pools

Jareño

Ortega-Prieto

Díaz-Martínez

et al. 2020

Preprint

Self Cite

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“…Two hundred serial passages of HCV p0 in Huh-7.5 cells resulted in population HCV p200, which displayed a 2-to 3-fold increase in replicative fitness, as calculated from progeny production in single and serial infections, as well as from growth competition experiments (72,73). The high-fitness intermediate-passage HCV p100 and HCV p200 displayed a lower sensitivity to the anti-HCV agents than their parental virus, HCV p0, including to favipiravir and ribavirin (72,74,75), thus providing HCV populations for a stringent evaluation of synergistic activities. The infectious progeny production upon single infections of Huh-7.5 cells by HCV p0, HCV p100, and HCV p200 was 10-to 100-fold lower with favipiravir-ribavirin combinations than with the individual analogues ( Fig.…”

Section: Resultsmentioning

confidence: 99%

“…Cells, viruses, and infections. Huh-7.5 cells and Huh-7.5 reporter cells were grown in Dulbecco's modification of Eagle's medium (DMEM) at 37°C in 5% CO 2 as previously described (74,90,91). Huh-7.5 reporter cells were used for all infections in the absence and the presence of drugs, while Huh-7.5 cells were used for titration of infectivity.…”

Section: Methodsmentioning

confidence: 99%

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Synergistic Lethal Mutagenesis of Hepatitis C Virus

Gallego

Soria

Gregori

et al. 2019

Antimicrob Agents Chemother

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Lethal mutagenesis is an antiviral approach that consists of extinguishing a virus by an excess of mutations acquired during replication in the presence of a mutagenic agent, often a nucleotide analogue. One of its advantages is its broad-spectrum nature, which renders the strategy potentially effective against emergent RNA viral infections. Here we describe the synergistic lethal mutagenesis of hepatitis C virus (HCV) by a combination of favipiravir (T-705) and ribavirin. Synergy has been documented over a broad range of analogue concentrations using the Chou-Talalay method implemented in CompuSyn graphics software, with the average dose reduction index (DRI) being above 1 (68.02 ± 101.6 for favipiravir and 5.83 ± 6.07 for ribavirin) and the average combination indices (CI) being below 1 (0.52 ± 0.28). Furthermore, analogue concentrations that individually did not extinguish high-fitness HCV in 10 serial infections extinguished high-fitness HCV in 1 to 2 passages when used in combination. Although both analogues displayed a preference for G → A and C → U transitions, deep sequencing analysis of mutant spectra indicated a different preference of the two analogues for the mutation sites, thus unveiling a new possible synergy mechanism in lethal mutagenesis. The prospects for synergy among mutagenic nucleotides as a strategy to confront emerging viral infections are discussed.

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