Efficacy of Carraguard-based microbicides in vivo despite variable in vitro activity.

Efficacy of Carraguard-based microbicides in vivo despite variable in vitro activity.

Anti-HIV microbicides are being investigated in clinical trials and understanding how promising strategies work, coincident with demonstrating efficacy in vivo, is central to advancing new generation microbicides. We evaluated Carraguard and a new generation Carraguard-based formulation containing t...

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Main Authors: Stuart G Turville, Meropi Aravantinou, Todd Miller, Jessica Kenney, Aaron Teitelbaum, Lieyu Hu, Anne Chudolij, Tom M Zydowsky, Michael Piatak, Julian W Bess, Jeffrey D Lifson, James Blanchard, Agegnehu Gettie, Melissa Robbiani
Format: Article
Language:English
Published: Public Library of Science (PLoS) 2008-09-01
Series:PLoS ONE
Online Access:http://europepmc.org/articles/PMC2525816?pdf=render
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spelling doaj-b2e0ec5a9dda40b193d8963381ddb0732020-11-25T01:50:15ZengPublic Library of Science (PLoS)PLoS ONE1932-62032008-09-0139e316210.1371/journal.pone.0003162Efficacy of Carraguard-based microbicides in vivo despite variable in vitro activity.Stuart G TurvilleMeropi AravantinouTodd MillerJessica KenneyAaron TeitelbaumLieyu HuAnne ChudolijTom M ZydowskyMichael PiatakJulian W BessJeffrey D LifsonJames BlanchardAgegnehu GettieMelissa RobbianiAnti-HIV microbicides are being investigated in clinical trials and understanding how promising strategies work, coincident with demonstrating efficacy in vivo, is central to advancing new generation microbicides. We evaluated Carraguard and a new generation Carraguard-based formulation containing the non-nucleoside reverse transcriptase inhibitor (NNRTI) MIV-150 (PC-817). Since dendritic cells (DCs) are believed to be important in HIV transmission, the formulations were tested for the ability to limit DC-driven infection in vitro versus vaginal infection of macaques with RT-SHIV (SIVmac239 bearing HIV reverse transcriptase). Carraguard showed limited activity against cell-free and mature DC-driven RT-SHIV infections and, surprisingly, low doses of Carraguard enhanced infection. However, nanomolar amounts of MIV-150 overcame enhancement and blocked DC-transmitted infection. In contrast, Carraguard impeded infection of immature DCs coincident with DC maturation. Despite this variable activity in vitro, Carraguard and PC-817 prevented vaginal transmission of RT-SHIV when applied 30 min prior to challenge. PC-817 appeared no more effective than Carraguard in vivo, due to the limited activity of a single dose of MIV-150 and the dominant barrier effect of Carraguard. However, 3 doses of MIV-150 in placebo gel at and around challenge limited vaginal infection, demonstrating the potential activity of a topically applied NNRTI. These data demonstrate discordant observations when comparing in vitro and in vivo efficacy of Carraguard-based microbicides, highlighting the difficulties in testing putative anti-viral strategies in vitro to predict in vivo activity. This work also underscores the potential of Carraguard-based formulations for the delivery of anti-viral drugs to prevent vaginal HIV infection.http://europepmc.org/articles/PMC2525816?pdf=render
collection DOAJ
language English
format Article
sources DOAJ
author Stuart G Turville
Meropi Aravantinou
Todd Miller
Jessica Kenney
Aaron Teitelbaum
Lieyu Hu
Anne Chudolij
Tom M Zydowsky
Michael Piatak
Julian W Bess
Jeffrey D Lifson
James Blanchard
Agegnehu Gettie
Melissa Robbiani
spellingShingle Stuart G Turville
Meropi Aravantinou
Todd Miller
Jessica Kenney
Aaron Teitelbaum
Lieyu Hu
Anne Chudolij
Tom M Zydowsky
Michael Piatak
Julian W Bess
Jeffrey D Lifson
James Blanchard
Agegnehu Gettie
Melissa Robbiani
Efficacy of Carraguard-based microbicides in vivo despite variable in vitro activity.
PLoS ONE
author_facet Stuart G Turville
Meropi Aravantinou
Todd Miller
Jessica Kenney
Aaron Teitelbaum
Lieyu Hu
Anne Chudolij
Tom M Zydowsky
Michael Piatak
Julian W Bess
Jeffrey D Lifson
James Blanchard
Agegnehu Gettie
Melissa Robbiani
author_sort Stuart G Turville
title Efficacy of Carraguard-based microbicides in vivo despite variable in vitro activity.
title_short Efficacy of Carraguard-based microbicides in vivo despite variable in vitro activity.
title_full Efficacy of Carraguard-based microbicides in vivo despite variable in vitro activity.
title_fullStr Efficacy of Carraguard-based microbicides in vivo despite variable in vitro activity.
title_full_unstemmed Efficacy of Carraguard-based microbicides in vivo despite variable in vitro activity.
title_sort efficacy of carraguard-based microbicides in vivo despite variable in vitro activity.
publisher Public Library of Science (PLoS)
series PLoS ONE
issn 1932-6203
publishDate 2008-09-01
description Anti-HIV microbicides are being investigated in clinical trials and understanding how promising strategies work, coincident with demonstrating efficacy in vivo, is central to advancing new generation microbicides. We evaluated Carraguard and a new generation Carraguard-based formulation containing the non-nucleoside reverse transcriptase inhibitor (NNRTI) MIV-150 (PC-817). Since dendritic cells (DCs) are believed to be important in HIV transmission, the formulations were tested for the ability to limit DC-driven infection in vitro versus vaginal infection of macaques with RT-SHIV (SIVmac239 bearing HIV reverse transcriptase). Carraguard showed limited activity against cell-free and mature DC-driven RT-SHIV infections and, surprisingly, low doses of Carraguard enhanced infection. However, nanomolar amounts of MIV-150 overcame enhancement and blocked DC-transmitted infection. In contrast, Carraguard impeded infection of immature DCs coincident with DC maturation. Despite this variable activity in vitro, Carraguard and PC-817 prevented vaginal transmission of RT-SHIV when applied 30 min prior to challenge. PC-817 appeared no more effective than Carraguard in vivo, due to the limited activity of a single dose of MIV-150 and the dominant barrier effect of Carraguard. However, 3 doses of MIV-150 in placebo gel at and around challenge limited vaginal infection, demonstrating the potential activity of a topically applied NNRTI. These data demonstrate discordant observations when comparing in vitro and in vivo efficacy of Carraguard-based microbicides, highlighting the difficulties in testing putative anti-viral strategies in vitro to predict in vivo activity. This work also underscores the potential of Carraguard-based formulations for the delivery of anti-viral drugs to prevent vaginal HIV infection.
url http://europepmc.org/articles/PMC2525816?pdf=render
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