Exploiting the Anti-HIV-1 Activity of Acyclovir: Suppression of Primary and Drug-Resistant HIV Isolates and Potentiation of the Activity by Ribavirin

Vanpouille, C.; Lisco, Andrea; Introini, Andrea; Grivel, Jean‐Charles; Munawwar, Arshi; Merbah, Mélanie; Schinazi, Raymond F.; Derudas, Marco; McGuigan, Christopher; Balzarini, Jan; Margolis, Leonid

doi:10.1128/aac.05986-11

Cited by 17 publications

(15 citation statements)

References 42 publications

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“…Indeed, the effect of ACV on HIV VL was initially attributed to the suppression of HSV-2 replication followed by the suppression of HSV-2-triggered inflammation [48, 49]. However, we and others [30, 50, 51] have found that ACV also has a direct effect on HIV-1 after the drug is phosphorylated by HHV. The direct inhibitory effect of ACV on HIV VL observed ex vivo was recently confirmed in vivo in a double-blind crossover clinical trial [52].…”

Section: Discussionmentioning

confidence: 98%

A common anti-cytomegalovirus drug, ganciclovir, inhibits HIV-1 replication in human tissues ex vivo

Vanpouille

Bernatchez

Lisco

et al. 2017

Aids

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Cytomegalovirus (CMV) is a common HIV-1 copathogen. Since CMV infection is an important contributor to immune activation, the driving force of HIV disease, an anti-CMV strategy might be beneficial to HIV-infected patients. Shin et al. reported that anti-CMV therapy with valganciclovir in coinfected individuals results in a decrease of HIV viral load that is not accompanied by a decrease of immune activation. This suggests an alternative mechanism for HIV inhibition other than suppression of CMV-mediated inflammation. Here, we show that ganciclovir, the active form of valganciclovir, has a direct suppressive activity on HIV replication in human tissues ex vivo, including HIV-1 of laboratory strains, drug-resistant and primate isolates. We deciphered the mechanism of this inhibition and showed that GCV-TP is incorporated in the nascent DNA chain and acts as a delayed chain terminator.

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Section: Discussionmentioning

confidence: 98%

A common anti-cytomegalovirus drug, ganciclovir, inhibits HIV-1 replication in human tissues ex vivo

Vanpouille

Bernatchez

Lisco

et al. 2017

Aids

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“…The assay developed by Biancotto et al (Biancotto et al, 2009) using mAb 4F6 as a C-Ab has demonstrated a great ability to measure concentrations of HIV-1 belonging to B subtypes (Balzarini et al, 2013; Introini et al, 2013; Merbah et al, 2012; Parrish et al, 2013; Saba et al, 2010; Vanpouille et al, 2012); however, its capacity to measure p24 from multiple non-B samples was more limited and opened the door for an assay using a more universal C-Ab. Biancotto et al .…”

Section: Discussionmentioning

confidence: 99%

“…As for all immunological assays, the success relies on the avidity and specificity of the C-Abs selected. Biancotto et al (Biancotto et al, 2009) developed a sensitive assay for the detection of p24 using the Luminex technology that has been used in many HIV-1 subtype B studies (Balzarini et al, 2013; Introini et al, 2013; Merbah et al, 2012; Parrish et al, 2013; Saba et al, 2010; Vanpouille et al, 2012). However, the C-Ab described by Biancotto et al lacks sensitivity for some HIV-1 non-B subtypes which account for almost 90% of HIV-1 infections worldwide (Hemelaar et al, 2011).…”

Section: Introductionmentioning

confidence: 99%

Standardization of a cytometric p24-capture bead-assay for the detection of main HIV-1 subtypes.

Merbah

Onkar

Grivel

et al. 2016

Journal of Virological Methods

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The prevailing method to assess HIV-1 replication and infectivity is to measure the production of p24 Gag protein by enzyme-linked immunosorbent assay (ELISA). Since fluorescent bead-based technologies offer a broader dynamic range and higher sensitivity, this study describes a p24 capture Luminex assay capable of detecting HIV-1 subtypes A, B, C, D, circulating recombinant forms (CRF) CRF01_AE and CRF02_AG, which together are responsible for over 90% of HIV-1 infections worldwide. The success of the assay lies in the identification and selection of a cross-reactive capture antibody (clone 183-H12-5C). Fifty-six isolates that belonged to six HIV-1 subtypes and CRFs were successfully detected with p-values below 0.021; limits of detection ranging from 3.7 to 3×104 pg/ml. The intra- and inter-assay variation gave coefficient of variations below 6 and 14%, respectively. The 183-bead Luminex assay also displayed higher sensitivity of 91% and 98% compared to commercial p24 ELISA and a previously described Luminex assay. The p24 concentrations measured by the 183-bead Luminex assay showed a significant correlation (R = 0.92, p<0.0001) with the data obtained from quantitative real time PCR. This newly developed p24 assay leverages the advantages of the Luminex platform, which include smaller sample volume and simultaneous detection of up to 500 analytes in a single sample, and delivers a valuable tool for the field.

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“…HIV-1 p24 gag concentrations were 49 ± 3 ng/ml and 53 ± 3 ng/ml for HIV-1 BaL and HIV-1 LAI.04 stock, respectively. For more viral preparations used in our experimental setting see References 3 and 4.…”

Section: Materials and Reagentsmentioning

confidence: 99%

An ex vivo Model of HIV-1 Infection in Human Lymphoid Tissue and Cervico-vaginal Tissue

Introini¹,

Vanpouille²,

Grivel³

et al. 2014

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Exploiting the Anti-HIV-1 Activity of Acyclovir: Suppression of Primary and Drug-Resistant HIV Isolates and Potentiation of the Activity by Ribavirin

Cited by 17 publications

References 42 publications

A common anti-cytomegalovirus drug, ganciclovir, inhibits HIV-1 replication in human tissues ex vivo

A common anti-cytomegalovirus drug, ganciclovir, inhibits HIV-1 replication in human tissues ex vivo

Standardization of a cytometric p24-capture bead-assay for the detection of main HIV-1 subtypes.

An ex vivo Model of HIV-1 Infection in Human Lymphoid Tissue and Cervico-vaginal Tissue

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