Humanized Mice Recapitulate Key Features of HIV-1 Infection: A Novel Concept Using Long-Acting Anti-Retroviral Drugs for Treating HIV-1

BACKGROUND: Humanized mice generate a lymphoid system of human origin subsequent to transplantation of human CD34+ cells and thus are highly susceptible to HIV infection. Here we examined the efficacy of antiretroviral treatment (ART) when added to food pellets, and of long-acting (LA) antiretrovira...

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Autores principales: Nischang, Marc, Sutmuller, Roger, Gers-Huber, Gustavo, Audigé, Annette, Li, Duo, Rochat, Mary-Aude, Baenziger, Stefan, Hofer, Ursula, Schlaepfer, Erika, Regenass, Stephan, Amssoms, Katie, Stoops, Bart, Van Cauwenberge, Anja, Boden, Daniel, Kraus, Guenter, Speck, Roberto F.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2012
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3374767/
https://www.ncbi.nlm.nih.gov/pubmed/22719966
http://dx.doi.org/10.1371/journal.pone.0038853
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author Nischang, Marc
Sutmuller, Roger
Gers-Huber, Gustavo
Audigé, Annette
Li, Duo
Rochat, Mary-Aude
Baenziger, Stefan
Hofer, Ursula
Schlaepfer, Erika
Regenass, Stephan
Amssoms, Katie
Stoops, Bart
Van Cauwenberge, Anja
Boden, Daniel
Kraus, Guenter
Speck, Roberto F.
author_facet Nischang, Marc
Sutmuller, Roger
Gers-Huber, Gustavo
Audigé, Annette
Li, Duo
Rochat, Mary-Aude
Baenziger, Stefan
Hofer, Ursula
Schlaepfer, Erika
Regenass, Stephan
Amssoms, Katie
Stoops, Bart
Van Cauwenberge, Anja
Boden, Daniel
Kraus, Guenter
Speck, Roberto F.
author_sort Nischang, Marc
collection PubMed
description BACKGROUND: Humanized mice generate a lymphoid system of human origin subsequent to transplantation of human CD34+ cells and thus are highly susceptible to HIV infection. Here we examined the efficacy of antiretroviral treatment (ART) when added to food pellets, and of long-acting (LA) antiretroviral compounds, either as monotherapy or in combination. These studies shall be inspiring for establishing a gold standard of ART, which is easy to administer and well supported by the mice, and for subsequent studies such as latency. Furthermore, they should disclose whether viral breakthrough and emergence of resistance occurs similar as in HIV-infected patients when ART is insufficient. METHODS/PRINCIPAL FINDINGS: NOD/shi-scid/γ(c)null (NOG) mice were used in all experimentations. We first performed pharmacokinetic studies of the drugs used, either added to food pellets (AZT, TDF, 3TC, RTV) or in a LA formulation that permitted once weekly subcutaneous administration (TMC278: non-nucleoside reverse transcriptase inhibitor, TMC181: protease inhibitor). A combination of 3TC, TDF and TMC278-LA or 3TC, TDF, TMC278-LA and TMC181-LA suppressed the viral load to undetectable levels in 15/19 (79%) and 14/14 (100%) mice, respectively. In successfully treated mice, subsequent monotherapy with TMC278-LA resulted in viral breakthrough; in contrast, the two LA compounds together prevented viral breakthrough. Resistance mutations matched the mutations most commonly observed in HIV patients failing therapy. Importantly, viral rebound after interruption of ART, presence of HIV DNA in successfully treated mice and in vitro reactivation of early HIV transcripts point to an existing latent HIV reservoir. CONCLUSIONS/SIGNIFICANCE: This report is a unique description of multiple aspects of HIV infection in humanized mice that comprised efficacy testing of various treatment regimens, including LA compounds, resistance mutation analysis as well as viral rebound after treatment interruption. Humanized mice will be highly valuable for exploring the antiviral potency of new compounds or compounds targeting the latent HIV reservoir.
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spelling pubmed-33747672012-06-20 Humanized Mice Recapitulate Key Features of HIV-1 Infection: A Novel Concept Using Long-Acting Anti-Retroviral Drugs for Treating HIV-1 Nischang, Marc Sutmuller, Roger Gers-Huber, Gustavo Audigé, Annette Li, Duo Rochat, Mary-Aude Baenziger, Stefan Hofer, Ursula Schlaepfer, Erika Regenass, Stephan Amssoms, Katie Stoops, Bart Van Cauwenberge, Anja Boden, Daniel Kraus, Guenter Speck, Roberto F. PLoS One Research Article BACKGROUND: Humanized mice generate a lymphoid system of human origin subsequent to transplantation of human CD34+ cells and thus are highly susceptible to HIV infection. Here we examined the efficacy of antiretroviral treatment (ART) when added to food pellets, and of long-acting (LA) antiretroviral compounds, either as monotherapy or in combination. These studies shall be inspiring for establishing a gold standard of ART, which is easy to administer and well supported by the mice, and for subsequent studies such as latency. Furthermore, they should disclose whether viral breakthrough and emergence of resistance occurs similar as in HIV-infected patients when ART is insufficient. METHODS/PRINCIPAL FINDINGS: NOD/shi-scid/γ(c)null (NOG) mice were used in all experimentations. We first performed pharmacokinetic studies of the drugs used, either added to food pellets (AZT, TDF, 3TC, RTV) or in a LA formulation that permitted once weekly subcutaneous administration (TMC278: non-nucleoside reverse transcriptase inhibitor, TMC181: protease inhibitor). A combination of 3TC, TDF and TMC278-LA or 3TC, TDF, TMC278-LA and TMC181-LA suppressed the viral load to undetectable levels in 15/19 (79%) and 14/14 (100%) mice, respectively. In successfully treated mice, subsequent monotherapy with TMC278-LA resulted in viral breakthrough; in contrast, the two LA compounds together prevented viral breakthrough. Resistance mutations matched the mutations most commonly observed in HIV patients failing therapy. Importantly, viral rebound after interruption of ART, presence of HIV DNA in successfully treated mice and in vitro reactivation of early HIV transcripts point to an existing latent HIV reservoir. CONCLUSIONS/SIGNIFICANCE: This report is a unique description of multiple aspects of HIV infection in humanized mice that comprised efficacy testing of various treatment regimens, including LA compounds, resistance mutation analysis as well as viral rebound after treatment interruption. Humanized mice will be highly valuable for exploring the antiviral potency of new compounds or compounds targeting the latent HIV reservoir. Public Library of Science 2012-06-13 /pmc/articles/PMC3374767/ /pubmed/22719966 http://dx.doi.org/10.1371/journal.pone.0038853 Text en Nischang et al. http://creativecommons.org/licenses/by/4.0/ This is an open-access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are properly credited.
spellingShingle Research Article
Nischang, Marc
Sutmuller, Roger
Gers-Huber, Gustavo
Audigé, Annette
Li, Duo
Rochat, Mary-Aude
Baenziger, Stefan
Hofer, Ursula
Schlaepfer, Erika
Regenass, Stephan
Amssoms, Katie
Stoops, Bart
Van Cauwenberge, Anja
Boden, Daniel
Kraus, Guenter
Speck, Roberto F.
Humanized Mice Recapitulate Key Features of HIV-1 Infection: A Novel Concept Using Long-Acting Anti-Retroviral Drugs for Treating HIV-1
title Humanized Mice Recapitulate Key Features of HIV-1 Infection: A Novel Concept Using Long-Acting Anti-Retroviral Drugs for Treating HIV-1
title_full Humanized Mice Recapitulate Key Features of HIV-1 Infection: A Novel Concept Using Long-Acting Anti-Retroviral Drugs for Treating HIV-1
title_fullStr Humanized Mice Recapitulate Key Features of HIV-1 Infection: A Novel Concept Using Long-Acting Anti-Retroviral Drugs for Treating HIV-1
title_full_unstemmed Humanized Mice Recapitulate Key Features of HIV-1 Infection: A Novel Concept Using Long-Acting Anti-Retroviral Drugs for Treating HIV-1
title_short Humanized Mice Recapitulate Key Features of HIV-1 Infection: A Novel Concept Using Long-Acting Anti-Retroviral Drugs for Treating HIV-1
title_sort humanized mice recapitulate key features of hiv-1 infection: a novel concept using long-acting anti-retroviral drugs for treating hiv-1
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3374767/
https://www.ncbi.nlm.nih.gov/pubmed/22719966
http://dx.doi.org/10.1371/journal.pone.0038853
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